A Non-Statin Pill That Really Lowers Cholesterol, Blood Pressure and Inflammation without Side Effects Would be a Good Investment, Right?[Ed. Note: Dr. KSS writes about medical topics and biotech stocks for the Irregulars. He has agreed to our trading restrictions, and his thoughts and words are his own. Enjoy!]
Any discussion of cholesterol immediately turns Brobdingnagian, such are the extremes in question.
Statins, which lower LDL cholesterol, are bombastically the best-selling drugs of all time. They’ve left a Paul Bunyan-size footprint in medicine. But they are hardly ancient and hoary. The prototype statin was discovered by Akira Endo, PhD, in 1970 while he worked for Japanese chemical giant Sankyo. Despite the Saganesque billions and billions of dollars, euros and yen his discoveries fetch every year, Endo has never seen even a nickel of the profits. Endo has been mildly honored, while those acting on principles he first introduced to the world, such as Brown and Goldstein, have gone on to Nobel notoriety.
Endo began with a hunch: cholesterol is an elemental life-cycle molecule for many organisms, and so maybe other organisms had stumbled onto ways to knock the cholesterol underpinnings out from potential invading pathogens as a safety measure. The fungi, for example, are famous sources of antibiotics that snuff bacteria. Maybe fungi had also devised a way to attack cholesterol production as a defense? Fungi have ergosterol rather than cholesterol in their cell membranes, and so could poison cholesterol-making machinery at no harm to themselves.
I’ve lived in Asia, and so have often searched for analogies to help Westerners understand how sharply Asian cultures differ from each other. One archetype is a thought exercise in which a representative of an Asian nation is given an uncut loaf of bread and asked to slice it in a way that reflects his/her culture. A Thai person, for example, would slice it ornately, lovingly, and so beautifully you’d be reluctant to eat it. A Vietnamese person would have it all sliced for you by the time you are finished explaining what you want. A Japanese person would devise a way to make bread slices that are but a few molecules thick. No culture has the fixity of purpose and ruthless attention to microscopic painstaking detail that the Japanese have. Endo went after this issue like a good Japanese scientist, and personally screened 6,000 individual compounds that had been purified from various fungi for one that could inhibit cholesterol synthesis. He didn’t have a high-throughput nanosensor-based microchip array to do it for him. He rolled up sleeves, told his wife not to wait up, and did it the old fashioned way.
Dr. Akira Endo, discoverer of statins
Endo’s work led to identification of monacolin K, later dubbed lovastatin, the first such agent used as a drug, in certain oyster mushrooms and other species of fungi. To this day, many statins used as drugs are purified from fermenting yeast rather than synthesized. Although the fungus-derived statins are natural products, somehow patent protection on them was finagled (now lapsed). Meanwhile, in its most legendary abuse of power, the FDA in 1998 tried to ban red yeast rice because it naturally contains lovastatin, made by the yeast. All statins are inhibitors of a liver enzyme called hydroxymethylglutaryl CoA reductase. 85-90 per cent of the body’s total cholesterol burden is made in liver, which is why the weak anti-cholesterol agent ezetimibe, which only blocks absorption of dietary cholesterol, has little effect and really does not warrant clinical use as it is not cost-effective.
The Brobdingnagian thing, again: no topic incites more vigorous discussion, more one-off hyperbole, than statins. Character X emerges from stage left to say he knows someone who lived to be 100, ate bacon and fried eggs for breakfast every morning, and never took any pills. Mrs. Y flies out of stage right to say that one dose was all it took…..a statin nearly killed her husband and she can prove it. A chorus begins a strophe: “We’ll all get muscle aches anon!,” though perhaps only a fourth of statin users get meaningful muscle pain. Offstage a mournful basso begins a lacrimae about how his best friend took statins every day just like the doctor ordered and they didn’t save him from The Big One. I’ve posted commentaries on them, as has Michael Jorrin, and invariably the threads that follow become tempestuous. Many readers are angered by their doctors’ glib default recommendations that all should be on them and others assert their exceptional wellness in the absence of, or because of the absence of, a statin prescription. Statins are blockbuster drugs, and are so avidly believed in by both the medical and pharma establishments (which rarely are so aligned) that some only half-jokingly think statins should be in the water supply.
Even so, statins have their vigorous detractors, many of whom are quite learned. The International Network of Cholesterol Skeptics makes interesting if insufficient arguments. Every major medical credo always has passionate critics; Peter Duesberg, PhD, of UC-Berkeley has actively, savagely denied for 30 years that HIV causes AIDS. Duesberg is a member of the National Academy of Sciences. Statins are roundly bashed by abominations like Dr. Joseph Mercola at his appalling website, and commonly if people do quite the opposite of what Mercola asserts they should, they will be far better off and healthier. Mercola’s interests are not, of course, in health; they’re—-you guessed it!—-pecuniary! He tells you that health comes only from what he sells you, from his special nostrums that the establishment denies exist.
Where cooler heads prevail about vascular disease, the following large tenets usually emerge, on the basis of large numbers of studies of large numbers of people for large numbers of years:
(1) there is great merit to linking cholesterol with vascular disease. It is not the only factor, as insulin resistance, blood pressure and inflammation play roles too, but it is a major factor.
(2) statins are poorly tolerated in some patients, but by no means all. Most can muddle through, especially if they dose their statins at night and sleep through the muscle-ache interval.
(3) statins may not provide be-all-end-all vascular disease prevention because they address only the cholesterol aspect, but they do play a vital role, as the overpowering evidence is that cholesterol contributes to vascular disease and is easily modified.
(4) statins are definitively, overwhelmingly helpful in secondary prevention: preventing a second MI or CVA after a patient has had a first one. For primary prevention, helping a patient never have an initial event, their merit is debated still. The bulk of data shows them helpful in primary prevention, but that data is not as stark as for secondary prevention.
(5) statins do have other effects: they may worsen insulin resistance in some patients, intensify dementia in others (cholesterol is the most abundant substance in brain), though they clearly have mild anti-cancer effects. Occasionally statins can trigger a syndrome called rhabdomyolysis. I have managed several people through it: rhabdo is ugly, painful (it is a breakdown and profound inflammation of muscle tissue), leads to renal failure. Not only are statins not ideal, but the potential for significant problems from them is always just on the other side of the door.
Many people rightfully wonder: if cholesterol is so deleterious for humans, why has nature endowed us with so much of it? I would respond to this by stealing a line from Baruch Spinoza, that nature does not work with the end in view. Natural selection caters mostly to reproductive fitness, and so rigs us to be at our best until such time as we can reproduce. In slightly balder terms, nature may not care about what becomes of us beyond the age of 18 or so. We are configured and calibrated in fact so that two systems tend to get us into trouble: the clotting system and the lipid system. Both may be teed up to favor survival advantages for hunter-gatherers. If being attacked by a lion or cheetah is a daily threat, then you need to be able to clot your wounds quickly, and also channel to them ingredients needed to rebuild flesh. These abilities to clot and generate flesh become maladaptive for us as we age. An unfortunate additional feature of cholesterol metabolism has to do with how it interdigitates with other metabolic pathways, and somehow, the factors that drive weight gain, high blood pressure and inflammation all tend to make blood more coagulable and cholesterol more abundant in it.
Blood from a patient with profound familial hyper-cholesterolemia
In November 2013, the American Heart Association and American College of Cardiology issued new guidelines for prevention of MI and stroke. Their guidelines were that there is no longer a role for niacin, fibric acid derivatives (ie, clofibrate), bile acid sequestrants (ie, colesevelam), ezetimibe or fish oils. The reasoning was that even if any of these latter agents modify cholesterol parameters favorably, they do not lead to better outcomes for patients. This observation calls into question the whole cholesterol model of vascular disease, of course, and caused some to speculate that perhaps statins have effects beyond their role in lowering cholesterol. At any rate, the councils recommended statins for all, and this immediately led to cries of outrage in some circles, as there were claims of conflicts of interest: many members of the committee advancing statins had consulting and investigative ties to Big Pharma. There’s just one problem with that theory, however: with the exception of Astra-Zeneca’s (AZN) Crestor, statins are largely no longer patent-protected.
Scenario: Pfizer (PFE) loses patent protection on bestseller statin Lipitor. It has seemingly only one flagship product, Viagra, which is amazingly patent-protected til 2020, though Teva (TEVA) is allowed to launch a rival in 2017. PFE makes overture to buy AZN for the benefits of tax inversion. And because AZN’s Crestor is still on patent til mid-2016, it gets rebuffed. PFE’s R&D pipeline is fallow, and PFE is smarting from a fall off a patent cliff. What can it do to right its ship? In fact, what can Big Pharma do to put shareholders back on the gravy strain of dividends and profits to rival the statin golden years?
And what can medicine devise to really prevent heart attacks and strokes in people in such an effective and safe way that people no longer quibble over the cholesterol hypothesis and the imperfectness of statins?
A company I’ve found may hold the answer to these issues. And that may provide a surprise, an upset, to what many will think is a refutation of my thesis. But I will get to that shortly.
Statins mainly work by lowering LDL cholesterol. They inhibit the hepatocyte cholesterol synthesis enzyme HMG CoA reductase. Other present agents reduce LDL to a much lesser degree, raise HDL somewhat, lower triglycerides…..but do nothing to prevent cardiac and cerebrovascular events. And yet HMG CoA reductase is by no means the only enzyme pivotal for cholesterol synthesis. Why has no biotech entity tried some other means of blocking the production of cholesterol in liver?
Enter Esperion Therapeutics (ESPR) of Ann Arbor, Michigan. Esperanza is “hope” in Spanish, in which esperar means “to wait.” ESPR has many investors waiting hopefully for what may be some very nice news during the next six months regarding its main pipeline agent ETC-1002. Esperion had its IPO debut in mid-2013, when 17 insiders bought 3.4 million shares.
Aisling Capital (an investor in Durata (DRTX)), Domain Associates (investors in DRTX, Achaogen (AKAO) and Regado (RGDO)) and Alta Partners each own 2.1 million shares of ESPR. Roger Newton, PhD, Esperion’s founder and Chief Scientific Officer, owns 629,700 shares, the largest position of any company insider; Newton is also on ESPR’s board. Newton has chops and street cred: he co-discovered atorvastatin (PFE’s Lipitor, which PFE acquired Warner-Lambert for), and led its clinical development. Newton was once Brobdingnagianly called “The Luckiest Guy in the Drug Business” by Forbes Magazine.
Dr. Roger Newton, founder of Esperion
Esperion’s float is 13.5 million shares, 81 per cent of which are owned by institutions, and 93 per cent of which are owned by large-block holders. Its recent market capitalization is just under $250 million. Pfizer owns nearly 6 per cent of Esperion, and no other pharmaceutical company has a position in it. Pfizer has some history with Esperion, which I will discuss.
ETC-1002 is being developed because it inhibits ATP citrate lyase, a fundamental step in cholesterol biosynthesis. Curiously, however, ETC-1002, which is an oral small molecule, also strongly activates 5′-adenosine monophosphate-activated protein kinase (AMPK). AMPK has important roles, or seems to, in insulin sensitivity, inflammation, weight, and even blood pressure. ESPR has preliminary clinical evidence of improvement in all four of those parameters in ETC-1002-treated patients.
The primary basis of statin-intolerance is that a minority of patients unpredictably have defects or mutations in an anionic transporter molecule that is responsible for uptake of statins into liver cells. In patients so afflicted, muscle tissue sees undue burdens of statin, which is toxic to muscle tissue. ETC-1002 is taken up into liver by a different mechanism, and in fact in a sizable cluster of phase 1 and phase 2 trials has yet to cause any serious adverse events and only rarely leads to minor instances of side effects.
ATP citrate lyase is an enzyme that merits some technical attention. It is found in cell cytosol, as opposed to nucleus, mitochondria, endoplasmic reticulum or lysosome. As described in this helpful recent review article, which has an excellent diagram of reactions on page 2, ATP citrate lyase generates acetyl CoA from citrate, which then has one of three fates: it feeds into cholesterol synthesis (HMG CoA reductase, inhibited by statins, is the very next step), or fatty acid synthesis (which means inhibiting the enzyme could result in triglyceride reduction), or else into acetylation reactions, such as those of histones, which bind DNA. Histone deacetylase modulators are a “hot” area in cancer therapeutics, and in fact an abundance of evidence shows that inhibiting ATP citrate lyase blocks tumorigenesis.
You’re bound to be wondering: does ETC-1002 work? Does it lower LDL cholesterol?
Esperion presented a fine poster at the 2014 National Lipid Association that meta-analyzed 4 phase 2a studies of ETC-1002: placebo-controlled dose escalation studies of the drug in patients with dyslipidemia, with dyslipidemia and type II DM, and dyslipidemia with statin intolerance, and in addition to atorvastatin. You can review the data here. But the key summary points are that LDL lowering was dose-dependent, was much more prominent in patients with diabetes, was well-tolerated, and above all else, achieved LDL reductions comparable to what statins can achieve. Bear in mind: this effect is additive to statins and possibly synergistic. In fact, one can envision a future in which a patient might not be placed on either a statin or ETC-1002, but on both, and with a reduced dose of statin so that side effects are milder. A common goal of statin therapy is reduction of LDL to 100 mg/dL or less, and from these studies it appears this is easily accomplished in a brief time with 240 mg ETC-1002 once daily. Some patients on ETC-1002 have achieved 80 per cent diminutions in LDL cholesterol.
Among the most interesting findings in these studies is that ETC-1002 therapy afforded reductions in hsCRP, a marker of inflammation, of 40 per cent or more as compared with placebo. This is a striking and statistically significant finding. While statins do lower hsCRP to a degree, this effect in them has been less comprehensively studied. In these trials, ETC-1002 was no likelier than placebo to lead to any adverse event, something statins can never claim.
In another pooled analysis, Esperion has demonstrated that ETC-1002 establishes a nearly 7 mm Hg reduction in blood pressure with statistical significance. The mechanism of this is not yet known, but the effect is additive to other anti-hypertensives, and is certainly a physiological benefit none of the statins can boast. The links to the posters provide ample graphics supporting the data.
Esperion is now enrolling in two phase 2b studies. One examines ETC-1002 as an add-on to ongoing statin therapy. It is placebo-controlled, and compares two doses of ETC-1002, and seeks 132 patients among 27 U.S. study locations. The other examines ETC-1002 in 144 patients with both hypercholesterolemia and hypertension at 35 U.S. centers. This latter study will of course examine achievement of blood pressure reduction goals. Both studies have a mix of urban and rural, private and academic study sites. Both will also look at effects on LDL particle size, number and distribution, apolipoprotein B, and HDL cholesterol, as some evidence has suggested Esperion’s drug may slightly lower HDL.
For would-be investors in Esperion, as for the company, the main question is not whether to proceed to a large phase 3 trial, but rather what sort of phase 3 should be run. Here Esperion is feeling its way. The goals of such a trial must be clearly decided in advance: is ETC-1002 to be studied as a stand-alone lipid-lowering agent, in which case it might be compared with placebo? Or would the FDA deem statins to be standard of care and so insist on a head-to-head trial against statins? Or does the company wish to pursue an add-on, adjunctive indication in which the drug can be used in addition to statins, recognizing that some physicians will prescribe it as stand-alone therapy? This will take careful decision analysis, and deft negotiation with the FDA. No single class of drug has been as comprehensively studied in human trials as the statins have. The tenor and expectations of such negotiations, however, may be strongly affected by the fact we are now nearly in a post-brand-name statin era. Since ETC-1002 works by a route completely untouched by statins, the FDA may well endorse development along two paths (both as single-agent therapy and as adjunctive therapy).
At the same time, Esperion does face a serious obstacle in that statins have been so thoroughly studied. In fact statins appear to have vascular protective effects that may be unrelated to either their lipid-lowering or inflammation-lowering abilities. The most cited and best study in this regard is the 20,000-patient 5-year study that appeared in The Lancet in 2011. Patients lacking elevations in LDL and hsCRP were just as likely as patients with elevations to be protected from MI and CVA. The ability of statins to lower hsCRP is not related to their effects on cholesterol, and meanwhile many antihypertensive agents have anti-inflammatory effects. My feeling is that it would be most unfortunate if the FDA required Esperion to compare ETC-1002 in a head-to-head way with statins, as it could shine nicely as monotherapy in the statin-intolerant, and as add-on treatment in those with an insufficient statin response. My sense is that ETC-1002 more potently lowers hsCRP than statins do, but I cannot prove that, and the two have never been directly compared.
One tricky aspect of ETC-1002’s development may be that the FDA will want data not only of LDL reduction, but also of event risk reduction too. We now know that non-statins that improve lipoprotein profiles make no difference in MI and stroke risk. ETC-1002’s case is strongly enhanced by the fact that it sharply lower hsCRP, a great bonus. But evidence-based medicine insists on evidence, and the fact is that these markers are imperfect surrogates for risk reduction. Accordingly, it is very possible that Esperion will be placed into performing risk-reduction phase 3 trials to support an NDA for ETC-1002. Such trials would be quite expensive, and unless the company is acquired, will warrant dilutive capital-raising. Pfizer may be looking for acquisitions to bulk up its pipeline, and would be a good fit with Esperion, but at the same time may wish to devote energy to bigger transformative steps than acquiring a microcap company.
Some company history is worth mentioning. Before the present Esperion was formed in 2008, there was a prior incarnation of Esperion, which developed ETC-1002 in 2004. That Esperion was acquired totally by Pfizer. ESPR in current form broke away from Pfizer, and purchased from Pfizer worldwide rights to ETC-1002, and does not have to pay licensing fees or royalties to Pfizer in any form. Esperion’s relationship with Pfizer is amicable, and Pfizer owns ESPR shares. Is Pfizer actively thinking of buying out Esperion? That’s hard to know. Pfizer seems more concerned right now with a grandiose deal, such as a tax inversion, to reinvent itself. Even so, Esperion would be a diminutive company for it to acquire, and this would not confound larger plans. An Esperion acquisition however would fly in the face of the development resources Pfizer has placed behind its PCSK9 agent. Accordingly, a suitor might take the form of a another traditional pharma house, not a biotech.
The potential refutation to any investor interest in Esperion may be the coming of the PCSK9-acting agents.
Let’s discuss them.
It would be difficult for me to convey fully the extent to which I regard the advent of the PCSK9 inhibitors with boredom. Although Regeneron (REGN) and Sanofi (SNY) unveiled awaited data on 30 July that their new PCSK9-inhibiting monoclonal antibody alirocumab not only lowers cholesterol potently but also reduces cardiovascular event risk, investors seem to be forgetting key things about this class of drug, which includes Amgen (AMGN)‘s evolocumab and PFE‘s bococizumab (which lags the other two in development):
(1) these are injected drugs
(2) these drugs are not yet approved
(3) these drugs lower LDL cholesterol to such a stark degree that dementia may prove to a be a serious consequence of them. Make no mistake about it: “fuzzy thinking” is already pegged as a serious issue in PCSK9-antibody treated patients.
(4) therapy with these drugs will likely be priced at $10,000 or more per annum, which will create a third-party payer cost apocalypse that will make the everybody-can-recite $84,000 for 12 weeks of Gilead‘s (GILD) Sovaldi seem penny-ante. Although only 9 per cent of HCV-infected Americans have been cured, the fact is that they are cured by treatment, and do not require chronic intervention. And their numbers (“only” 3.2 million Americans have HCV) are utterly dwarfed by the number of Americans with dyslipidemia.
(5) the PCSK9 inhibitors will not replace statins, but will be used as add-ons. They will replace statin therapy only in those who have experienced clinical catastrophes on statins, which are rare.
Because of these considerations, drug companies expecting a register-ringing Hemingwayesque Moveable Feast of revenues from the PCSK9 inhibitors may be misguided. Your insurance company is not going to let you receive them just because you don’t like statins. And if the cognitive side effects are as bad as some suggest, you may not want to take them.
While the biochemistry of PCSK9 is complex, the Cliff’s Notes version is that it suppresses expression of the LDL receptor on the surface of hepatocytes. When PCSK9 is blocked by antibodies, LDL receptors are more abundant in liver, and so better able to soak up LDL from circulation. LDL is generally regarded as the entity that carries cholesterol to the arteries, while HDL is regarded as the conduit of cholesterol from arteries back to liver.
The whole PCSK9 monoclonal field had its legitimacy undermined when CNBC reporter Meg Tirrell broke a story on 30 July that Biomarin (BMRN) sold, for $67.5 million, a rare disease drug development voucher to Regeneron that will cut 4 months from its approval review cycle for alirocumab. This distasteful event reminds one of the ridiculousness of the sale of indulgences by the Catholic Church in the run-up to the Protestant Reformation. Drugs should be advanced on scientific merits, not certificated bribes. At fault here is neither REGN nor BMRN, but Margaret Hamburg’s FDA, which is quite OK with this abusive non-meritocratic practice, one it will likely make haste to place fig leaves over. It is because of kleptocratic practices like these that Sovaldi costs $1000 per pill. When I contemplate the drug development business in the US, “arch” and “turgid” and “epic” come to mind.
Most Irregulars who follow these biotech threads are now streetwise enough to realize that any time a drug works by blunting the effect of a protein, the same pharmaceutical effect can be achieved by using RNA silencing to suppress expression of the protein in question. To this end, Alnylam (ALNY) has already done phase I trials in the UK of a siRNA that silences expression of PCSK9. It’s unclear, however, that complete obliteration of PCSK9 is a good thing or a worthy goal, and Alnylam may be wishing to position itself to see how monoclonals to bind up PCSK9 fare before it advances itself into the lipid management arena. Alnylam has not presented phase I results, and most of its work in PCSK9 silencing is still preclinical.
Does Esperion have other attributes, other assets? It reports having acquired worldwide rights to an agent known as 4WF from Cleveland Clinic in 2011. 4WF is said to be an HDL mimetic, something that would channel lipid from areas of vascular disease back to liver, and the CSO has had an interest in these. Both 4WF and a second agent that seems to ameliorate hyperglycemia and weight in overfed mice, however, are strictly preclinical. Try as I might, I have been unable to glean any information about the molecular nature of these entities.
Then comes a question: is ETC-1002 something akin to a Second Coming of statins? I don’t know. What I can say for sure is that the PCSK9 inhibitors are not an event of eschatological significance, though Big Pharma wants us to believe that they are. ETC-1002 clearly has two strong effects in vivo, and sharply lowers both LDL cholesterol and inflammation as measured by hsCRP. It has few or minimal side effects, is compatible with other drugs and is far safer even at this stage of development than statins were ever known to be. Without resorting to hyperbole, ETC-1002 is a lot like a global metabolic tonic, one that tames the bundle of manifestations of syndrome X’s high cholesterol, high inflammation, high triglycerides, insulin resistance and high blood pressure. ETC-1002 could likely stand in the marketplace as either first- or second-line treatment for hypercholesterolemia. A vigorous search through the drug development literature suggests that no other viable oral-drug candidates for safe lowering of cholesterol are being trialled anywhere, and confirms that Esperion is in fact working along a unique mechanism and unique pathway (ATP citrate lyase), one that few know of, and one in which it has no competition at all. This is a drug indication littered with failures, and Esperion has made it past the worst of its hurdles, in my view. The architect of the strategy is the same person who brought the world Lipitor, the single best-selling cholesterol agent in history. He may be crafting another lipid home run.
ETC-1002 has completed 7 clinical trials now and done famously in all. Two new trials are underway, and the trial in patients with both high cholesterol and high blood pressure has just dosed its first patient. Data from both trials should be at hand no later than 2Q15, during which time, I suspect ESPR shares are likely to become less and less undervalued. Esperion isn’t the sort of recondite company trawling in sophisticated science that I usually delve into here, but it has a simple pill—one that works—-for mankind’s worst and most prevalent ailment, one that is likely to be sought after in an age where the best other pills no longer offer big profits. It is likely to be able to do so at prices that, unlike the costs of PCSK9 inhibitors, will not outrage pharmacy benefits managers. It’s an opportunity all the more compelling because of stealth. Seemingly no one knows of Esperion: no one has heard of it, and no one is familiar with the enzymic pathway it is acting on and the striking potency of its lead drug. We’ll be hearing more about ETC-1002 from Esperion and it’s likely to be good.
Is Esperion vulnerable to competition? Are others pursuing ATP citrate lyase inhibitors? I explored this in detail. A number of naturally-occurring molecules from fruits and vegetables, presumably not patentable, do inhibit ATP citrate lyase. Many other inhibitors exist as well, including halogen- and sulfur-substituted citric acid derivatives, the bile salt deoxycholic acid, vanadium, and even polychlorinated biphenyls. These moieties seem invariably to have one or more of the following issues: (1) severe toxicity, (2) severe side effects (e.g., radicicol is a good inhibitor, but a potent sedative), (3) unfavorable thermodynamics such that doses required would be enormous. These have been comprehensively reviewed in a 2012 paper by Zu and colleagues, and full pdf versions of this manuscript can be freely downloaded at researchgate.net. Above all else, none are even to clinical trials yet, and so Esperion has several years of lead time now.
Could Esperion be sideswiped by an RNAi company suppressing ATP citrate lyase expression? Others may try this, but bear in mind that this enzyme is life-critical, and that complete abrogation of it would likely be harmful. Also, Esperion’s drug acts by turning on the activity of the enzyme AMPK, something RNAi cannot do. Esperion’s drug candidate is a once daily pill that is well-tolerated, and since it appears to work well, it’s not likely to be supplanted by any form of injectable drug.
For more than a decade, cardiovascular disease researchers have conjectured widely about a “polypill”….a single tablet that might contain, for example, aspirin, a statin, a beta-blocker and an ACE inhibitor. The theory has been that compliance would be so good—all agents dosed once daily in one tablet; side effects minimal as the dose of each agent would be reduced; synergistic benefits among the drugs—that such a preparation could cut cardiovascular event risk by 75 per cent. ETC-1002 has so many health-positive actions (simultaneously lowering blood pressure, lipids, inflammation and cancer risk) that one cannot help but speculatively regard it as like a single-agent polypill: one drug, poly in its effects. Esperion knows this, and continues with phase 2b studies to limn and define the drug’s actions. As explored in this 2014 peer-reviewed study, ETC-1002’s metabolically favorable effects appear to shine in patients with type II DM. Phase 3 trials of ETC-1002 are unlikely to be underway until 3Q2015 at the earliest, but meanwhile my starter position in Esperion compels me to follow the company, track drug development, and be poised to add in anticipation of good news. The drug will probably never see an indication as a cancer preventive, of course, but Esperion can leverage the ample data on ATP citrate lyase inhibition’s anti-neoplastic effects as a means of currying favorable bias among patients.
In your due diligence, you’ll come across the company’s 2014 annual report, which confirms the fiscal health of Esperion. Analysts from Citi, Stifel Nicolaus, JMP Securities and Credit Suisse cover Esperion and all have “buy” or “strong buy” ratings on it.
Stock Gumshoe, of course, is not a tipsheet. For the many PhD and MD readers who now participate in this forum, I would encourage spending 1-2 hours to read over studies I have provided in hyperlinks, as you will find the content quite gratifying. It is intellectually sexy. Biopharma investing entails consummate risks, as although the body works along fixed principles, biology is bewilderingly complicated. Even so, if ever there were a biotech insider capable of pulling off a great second act in lipid drugs, Roger Newton is probably that person. Esperion is his company.
Addendum: The author owns shares in ESPR, PFE, GILD, AKAO, RGDO and DRTX, has no positions in any other mentioned company, and no plans to trade in any mentioned company for 7 days after publication.
This is a discussion topic or guest posting submitted by a Stock Gumshoe reader. The content has not been edited or reviewed by Stock Gumshoe, and any opinions expressed are those of the author alone.
Tim: Stubbings has a well-established tradition of not responding to any trigger-point query. He and French try to do a good cop bad cop routine with queries, with Stubbings being the bad guy. But when the query reminds Stubbings that he’s not going to be able to retire any time soon on his Benitec lottery winnings, he “didn’t get” that email. I have seen this many times with him. The company is insisting on running this trial itself, not using a CRO, to save money. Had a CRO been involved, a company that knows how trials are done and how to get them done, none of this fracas would be going on. Penny wisdom and pound foolishness. Based on what I am hearing, French is afraid there will be a palace coup…..and frankly that would be lovely for all of us holding shares. Pull up Benitec’s mgmt team. Then dart-throw and pick ANY US clinical stage biotech company’s mgmt team. You will notice a BIG difference. The US company will have MD’s and people with track records in getting drugs to market. Benitec has no one, but doesn’t think it has a problem.
The cacophony on Hot Copper owes in no small way to the fact that the average Australian biotech investor has about 5 per cent the sophistication of the average American one. I am not knocking Australia, but that is fact. The Australians invest in Oz biotech often for reasons of national pride, and that is a poor reason to invest in anything.
Biotech aside, this made my morning: ” the average Australian biotech investor has about 5 per cent the sophistication of the average American one.”
Thanks.
I’m in no way trying to incite or inflame, but isn’t Duke and UCSD the CRO? Aren’t the CRO’s the project managers? I’m confused by this as I thought that they in fact have a CRO.
I guess to be fair it depends on what is meant by CRO. Duke calls itself a “clinical research organization,” but what I meant was more along lines of “contract research organization.” Since the FDA doesn’t want study sponsors too intimately involved with study sites lest data integrity be compromised, the CRO is the go-between. Either the sponsor or the site can say things about the other to the CRO…things they wouldn’t want to say directly.
I have a transcript of a call someone made to Carl Stubbings in March. This caller was quite irked over failure to enroll, but is also quite a master of being hunky dory on the phone to people as their guts get ripped out by probing questions. Stubbings was getting more annoyed, and was ready to say something, say anything, to get this caller off his back. So he said (and if you read the words in context, you would realize…it is shamming, confabulation) at the very end, in a word searching way, that Dyook Medical had found a patient and he was sure the patient would be dosed “next week.” I felt this was a florid lie at the time, and events in the interim confirm it was a lie.
From an inside source, I knew Duke was getting tired of holding hands and changing diapers for Benitec. And so, I was concerned that Duke might refuse to go on with the study and so I said that if UCSD suddenly came on line, that would be a bad sign. But that doesn’t give the full perspective of what I felt: What a CEO with a sense of fiduciary responsibility would have done, long before 4.5 months had passed without a dosing, would have been to take action, issue PR and say something along lines of: “In order to pick up the pace of study execution, we have decided to bring online our second designated site at UCSD, as doing this will double our chance of finding a patient in the near term.” That he DID NOT do this, that he was willing for all of us to dangle and be angst-ridden for 4.5 months, is super-egregious and is a firing offense. It shows that his reality testing is not intact. So, basically this spring we got two breaches of fiduciary behavior by the two top C-suite people at Benitec.
In one of Martin Amis’s stories, a man and woman are wrangling with whether to break up after years together. We get interior monologues as to what the relationship has come to. Finally, one of the characters reasons: “You go when you can longer stay.” That is the point many Benitec longs now face. I am still long, and have sold nothing, and am sure I am blamed at Hot Copper for the share price fall, but I am not Zeus Apollo and do not control the winds or fate. Recent biotech history has brought many examples of CEO egregiousness…..the nonsense at Galena, for example, and the blatant lies at Provectus. Holladay (QRXPY) should be pilloried. But French is right up there with them, because failing to act is acting, failing to choose is choosing. Because of his (in)actions, that stock is at a third of its highs. My concern is that there is no intent to right the ship, because they don’t think things are amiss. They will point to their other projects…..WHAT PROJECTS? ALL flimsy arrangements no more substantive than pushpins on a map. Calling up a company like Regen or Biomics and cobbling together vague intent to do lunch sometime is NOT substantive action on behalf of shareholders!
Doc, thanks for your timely and thoughtful reply. I remain resolutely long. I think that K. Buchi is a great BOD member and his track record leaves me confident. The timelines are what seems to be upsetting so many shareholders and I for one am still OK with how things are playing out. Sure we all want data, data, data, but all in due time. We are in no danger of running out of cash as TT-034 is fully funded to completion. NSCLC could be where the company has to do another CR and that would be the time to re-evaluate. It is my belief that we will be able to fully finance the NSCLC without requiring another dilutive event once the data does indeed start flowing, but that remains to be seen.
If my memory serves me, there is the very real possibility we will see data that moves the needle by late ’14/1h15 and that time frame is fine with me.
Would we all have been happier if the SP never went so high (remember the gummy effect) ….it reached levels that it really didn’t deserve despite TKMR, ARWR etals MC’s that have since been slashed as well. Remember we are in a BRUTAL biotech environment. However, the thaw is already starting and I believe that we will benefit with the other boats that rise. Biotech has gotten destroyed. It will recycle back to being fairly valued and it is my belief that Benitec will be in a very good position to capitalize on the upturn in Biotech that is inevitably coming….unless they screw up this trial by compromising safety. The patients will become easier and easier to recruit as dose esculation increases which may in fact start to point to efficacy long before the end of the trial. Is it possible that MGMT knows they have a blockbuster and are playing this thing extremely close to the vest?
I respect and appreciate your perspective, believe that you have saved many people alot of money (except poor William Tweedie and his love of PVCT), given freely of your time, energy and expertise in answering many questions posted to you. However, I am going to respectfully disagree with you on PF for now. I just don’t see him as being nefarious, incompetent or otherwise worthy of scorn just yet. I just can’t lump him with Holladay, but understand that you are frustrated. I am giving him the benefit of the doubt and hope you may also reconsider. I remember you wrote an incredible piece back in late Jan early Feb defending MGMT and there deft handling of the FDA as well as their foresight in picking up Tacere for pennies on the dollar. Perhaps it was on HC but I remember the piece. I also remember the great rebuttal you wrote on the Kay paper. Please remember that you carry alot of weight in the Benitec community and I believe you will get your just rewards one day with a very hefty profit in this company, and a lot newly minted millionaire gummies will be very thankful for your introduction to the most exciting space in Biotech …..ddRNAi….Most will have you to thank, relax, this is not a QRXPY and you didn’t deserve the beating you took for it or RGDO. Please know that this is meant as praise for what you have done and my need to respectfully disagree with you on the PF subject for now. I will reevaluate if it becomes clear that things have gone off the rails. But for now I am staying put with Buchi and Suhy, just like you, and refuse to sell a single share.
Analog,
I appreciate your enthusiasm and your post. Don’t mean to speak for the doc but I think he believes French and Stubbings breached their fiduciary duties. If they did they should be gone. Delays may be inevitable, but after a while investors may be of the wrong ( or right) opinion that management is stalling. They may very well believe we have a blockbuster on our hands, but we need to prove it by completing trials. Again, while I share in your enthusiasm, companies either progress and grow, or stand still and get passed.
Tim,
Exactly who is going to pass them? ddRNAi is their IP…RNA therapy was set back a decade or more due to Jesse Gelsinger’s death. I will leave it to Buchi and the BOD to decide if fiduciary duties have been breached. But that is a huge leap on extremely shaky ground. I would be very much more concerned about a rushed, unsafe trial. So we don’t have another Gelsinger. Part of the reason for the incredibly positive FDA and NIH approvals were exactly because of the trial design that any investor should have read, understood the timelines, the reason for the escalations and cohorts designed as they were, before deciding to invest or invest too much that they follow every move and try to determine motives that simply don’t exist. We are barely out of infancy, not yet even a toddler and some expect this kid to already be enrolled in college. Buchi guided Cephalon through a 6Billion aquisition, he has a VERY vested interest in Benitec and is not going to let shareholders timelines determine the outcome of an FDA approved first in man trial of a non revocable injection therapy. People, including myself, bought at prices that simply were not yet sustainable. The SP is still way above my initial purchase price, +35%. When things change rapidly where do you want to be? On the bus or not? I will not sell until there is a fundamental change. And there has been none. Make no mistake, this trial is being watched very closely, shares have been guarded, obvious manipulation has occurred to wrest shares out of weak hands. There are only so many pieces of the pie and it is way too early in the game to throw breaches in fiduciary responsibility around. No doubt, if fiduciary duties were breached then they should be gone, but I simply see absolutely no evidence for that. None. They are listed on the ASX, not in the US. This is an extremely risky OTC stock not a blue chip. Things are being played extremely close to the vest. There are a lot of other companies that are in need of an examination for fiduciary irresponsibility, this is not one. Right now, with a patient dosed, a second to be dosed likely next week and transduction already occurred, what exactly do you want them to do? Data will come for god’s sake, just not on your timeline. I am sorry if this is causing stress, but how happy will you be when things come off properly, safety then efficacy is determined before the trial even ends. Did you really think this was going to explode before data comes in? A catalyst is likely to come out of the blue in the next 6-12mos. and you won’t have time to buy in. Hold and look at other things. Fretting over patient dosing delays accomplishes nothing. Delays are incredibly commonplace, occur for myriad reasons, and are going to be less and less likely as the second CRO is online and a lab is open being run by the very competent Dr. Suhy. Patients for the escalating doses will be very much easier to recruit.
When the FDA halts the trial over safety, Suhy or Buchi quits or some other negative catalyst occurs then I will be dead wrong. Will this occur anytime soon? I strongly doubt it. Please let’s wring our hands over something else.
NOTHING is more exciting right now in Biotech than ddRNAi… we are all blessed for the introduction to it by the good Dr. It will become a lot more commonly known in a very short amount of time in regards to the Biotech investing world. I mean it literally can take 7+ years to get a drug through a trial. However, a properly designed trial can receive breakthrough status. Data will come out within a year-18mos. showing a viral knockdown and patients that are alive and safe. Share prices could go to .20, I could care less as I have no hope of trading and timing this thing. When data is released showing things are going better than anyone could have hoped it will be impossible to get your hands on shares at a valuation that will be “blockbuster”. I truly hope that people are invested in this with a proper view of the horizon.
Analog,
Regarding your post 47,
You have every right for your opinion but let me cut to the chase. I respect many people on the board and am long ctix, snwr, and drtx thanks to the gummys. I have the utmost respect for Dr KSS and I believe him regarding his opinions on Benitec. Doesn’t mean I think it’s a blue chip stock. Doesn’t mean I have a 90 day time frame. Doesn’t mean I’m stressed. Doesn’t mean I’m one of the “weak sellers”. Doesn’t mean I don’t know biotech’s are having a tough year. Doesn’t mean I’ve stopped buying.
It does mean I believe Dr. KSS in his views on Benitec’s management and progress, I agree with him, and I’m frustrated and disappointed. Got it?
I don’t need to hear about Jesse Gellsinger or patience.
I waited out companies ( like F ) for many, many years for Gods sake. I will probably continue to voice my displeasure if I feel like it so don’t read it.
No need to be a$$holes to each other, guys. Let’s respectfully disagree here and in the end, we are all long Benitec anyway.
analog68 : Thanks for your recent posts on Benitec, Buchi and Suhi. I ‘LIKED’ your posts but definitely that was not enough to express my feelings when I read them.
Your thoughts were just what I had been feeling and thinking for a while, and there you expressed them much better than I ever could have.
Thanks for sharing and so glad you are part of this blog!
I would replace “investor” with “executives”.
Any comments on this S/A article this morning?
http://seekingalpha.com/article/2418705-benitecs-ddrnai-targeting-fight-against-hiv?uprof=46
I hate to admit it but I didn’t know there’s a lot of RNAi work going on around the world besides City of Hope, UCSD and Duke. Looks like good news. Comments please,
Cheers
Ken M.
Ken, English is clearly not Pannobhaso’s native language, and there’s nothing wrong with that, but English is the language of the medium in question, and he either needs to get help with it or stop writing in it, I find it to be very vapid writing lacking content and critical thinking. Only a fool would take seriously a Russian claim to be doing ddRNAi work on HIV (I may email that to a friend there so he can have a good bedtime bellylaugh). As always when I read one of PB’s pieces, I am never sure what his point is (if he has one). If he is trying to convey that ddRNAi is exciting, well, yeah, we know that. Tell us something we don’t. If he is trying to make the field of ddRNAi sound competitive vis a vis HIV, well, he doesn’t quite make that case, but for those to whom he does, it needlessly soft-pedals a long thesis in Benitec on a scientific basis. There IS no basis for that…..they have the best method, the best science. They just cannot/will not/don’t think they have to execute. It is too accustomed to being an armchair company. I have heard rumors they are paying far less attention now to bloggers, which is unfortunate, because I have continued posting things hoping my memes will infect people on the board and in the corporate office to DO something about the leadership vacuum at Benitec. The problem with being out of touch is that it is a non-proprioceptive state: you don’t know how out of touch you are. Australian investors are star-struck with this company from their young, small, ambitious nation because it is doing a study on High Street, in the US of A. Their expectations are being met, while ours are not even being touched.
Dr KSS
I, and I’m pretty sure everyone else, appreciates you trying to light a fire under French and Benitec. I bet he reads what is being said here, or he should, considering the anemic number of shares traded in the U.S. He’s gotta wonder why, doesn’t he? Can he have his head buried that far down in the sand? How long can he travel giving presentations, shaking hands, getting patted on the back, and being congratulated on his greatness? Dr. French, your Rome is burning due to inaction. It’s been almost 8 months since the FDA approved the study!
Tim I bought shares last summer on the basis of about 60 hours of due diligence over several weeks, and for the following reasons:
(1) excellence and implications of the science. It is the farthest thing from junk science you will encounter in this incarnation
(2) the plan to go from pre-clinical to being a clinical stage company
I like transforming events: change in company niche, arrival of company’s first good phase 2 or phase 3 data, for example, or company getting a first drug to market. These are the best places to invest, best yields.
(3) the company’s stated interest in what I would call “non-barbell” clinical goals. By that I mean that way too much biotech right now is clustered around the extremes: the orphan indications, or else the blockbuster indications. (By my definition, HCV is not blockbuster, though it is huge).
(4) its stated aims of getting more clinical people involved.
(5) the personal excitement I felt about how this trial would teach us volumes about HCV biology. So much remains not known about it, and I have devoted my life to fighting it.
But they are not progressing now on fronts 2, 3 and 4. I have growing concerns that 5 will never be fully realized, as I am not sure that the company can justify going to phase 2b/3 based on market conditions. It may stay as a demo study on the power of ddRNAi, on how it works, on what it can do, but not a planned clinical deployment of ddRNAi. I feel sorry for Suhy as I feel he is a good guy and scientist. This is his pet project, and it may never bear fruit. He is so deeply differentiated, career-wise, in ddRNAi, he cannot exactly walk away, and no pharma big cool friend will ever express an interest in ddRNAI until this company hits a proof home run on efficacy, safety and lack of off-target effects, as well as durability of effect. He is yoked to a somnambulist boss.
Your last sentence there, Doctor, reminds me…didn’t you or some other enlightened blogger recently suggest that Beni’s objective might be to just hang around while CalImmune, City of Hope et al PROVE ddRNAi, then simply issue licenses to entrepreneurs, sit back and cash the checks and never have to actually DO anything else?
Maybe it was just my imagination running wild OR I totally misunderstood the suggestion of others (a definite possibility).
Blessings all around,
Ken M.
Just to keep people oriented about Esperion ($ESPR):
Company plans to announce data from one key phase 2b study of its new agent in October (sooner than I had expected). I predict it will be positive.
Shares have been resilient the last few sessions. Long $ESPR.
Been looking at NVGN for months. Pulling trigger today. I have read at some point about the effficacy of targeting the cancer’s stem cell, their SBPs discussed below in the 6K filing cover this. The full 6K is a good read if you’re interested. Has sucessfully tested it’s low 2.75. Is 3.20 today. A low volume stock.
“About Novogen Limited
Novogen is a public, Australian drug-development company whose shares trade on both the Australian Securities Exchange (‘NRT’) and NASDAQ (‘NVGN’). The Novogen Group includes a New Haven CT-based joint venture company, CanTx Inc, with Yale University.
Novogen has two main drug technology platforms: super-benzopyrans (SBPs) and anti-tropomyosins (ATMs). SBP compounds have been created to have a uniform cytotoxic effect against both cancer stem cell and are being developed in the first instance for the treatment of ovarian cancer, neural cancers (glioblastoma, neuroblastoma) and prostate cancer. Cantrixil and Trilexium are SBP-based drugs. ATM compounds target the microfilament component of the cancer cell cytoskeleton and are being developed for the treatment of melanoma, neuroblastoma and prostate cancer with the rationale that a combined attack on both key components of the cytoskeleton (the microfilaments and the microtubules) delivers a comprehensive and permanent destruction of the cytoskeleton. ”
A liitle off our block, but I bought FONR today before the pop, around 12.00 now. They sell and also will manage their open MRIs which I would drive an extra mile to use and hold some good partents. http://www.fonar.com
Anything special shoving DRTX up today I should know about? I know they did a conference this morning…. It’s been slamming into the 200 day over the last week and wouldn’t go much lower so maybe a technical bounce/short squeeze? Anyhow, I’m enjoying it.
Hey Glenn, I cant recall if there are any concerns about Sanuwave’s finances. Are there concerns about dilution from a cash raising offering anytime soon?
Bradley,my thoughts on this is I think they have enough money to make it through dermaPace trial which if all goes well could be FDA approved sometime in mid 2015.
Company is totally focused on this trial money wise and I think has done a good job
on their spending .A ideal time for a secondary in my opinion would be after dermaPace
is FDA approved or if stock runs up high on upcoming data release in September.Either
way secondary would proabaly be done at a much higher price than what it is now.
Cheers,Glenn
Sorry for typo on probably,need to slow down.
Cheers,Glenn
If you are perusing financial news, don’t get fooled. Celadon got downgraded by analysts. That’s not our CelLadon ($CLDN).
I wanted to share an interesting resource: JP Morgan’s 2014 Global Biotech Outlook, that provides brief anayses of 50+ biotech stocks evaluated by JP Morgan teams. It’s a bit dated (compiled 8 months ago), but nevertheless an interesting read. Here is the link: https://www.jpmorgan.com/cm/BlobServer/JPM_2014_Global_Biotech__2014-01-06_1286305.pdf?blobkey=id&blobwhere=1320631529168&blobheader=application/pdf&blobheadername1=Cache-Control&blobheadervalue1=private&blobcol=urldata&blobtable=MungoBlobs
Let me know if the link fails, and I’ll try to re-structure it.
Link is good, thank you Lawrence! Good stuff!
timmuggs and all interested in Biotie,
Re your comment on Dr. KSS’s post #225 on Biotie, I’m posting a reply here instead of way back above. I don’t know which Biotie analysts Dr. KSS follows, but there are two listed on the Biotie website:
Edison Investment Research Limited, U.K. Here’s the link to their page on Biotie:
http://www.edisoninvestmentresearch.com/research/company/Biotie-Therapies-Corp
Edison’s analyst on Biotie, Christian Glennie, has positive things to say about its 2 main assets in this interview which is over 14 months old, written before UCB returned tozadenant to Biotie: http://www.thelifesciencesreport.com/pub/na/seven-biotech-options-that-buck-tradition-christian-glennie
The other analyst that Biotie’s webpage links to is Inderes Oy of Helsinki. Unfortunately, their website has no English option yet. Here’s a link to their rather comprehensive Initial Report on Biotie written last April, which is in English, quite long — 64 pages — but easy to read. I just found it yesterday & haven’t read it all myself yet. It’s positive (of course, or why would Biotie link it?), but points out lots of risk, and it assigned little value in April to their VAP-1 antibody against PSC, which Dr. KSS mentioned is soon to start a Phase 2 in the UK.
http://www.biotie.com/MATERIAALI_18%201%202011%20alkaen/SIJOITTAJAT%20SIVULLE/2014/Biotie_Initial_Report_23-4-14_Revised.pdf
This Initial Report on Biotie written by Inderes Oy’s analyst Juha Kinnunen lists several potential competitors to Biotie’s tozadenant for Parkinson’s Disease. Two or three of them are similar in that they also are inhibitors of the adenosine 2a (A2a) receptor and also for Parkinson’s sufferers. One in Japan has already been approved there: “Istradefylline has been marketed as the brand name NOURIAST® in Japan since May 30, 2013…(yet)… the FDA issued a non-approvable letter in February 2008.” Mr. Kinnunen said this about another one from Merck targeting the same adenosine 2a (A2a) receptor: “Pharma company Merck declared in May 2013 that it was going to discontinue the clinical program for preladenant, Merck’s investigational adenosine A2A receptor antagonist for the treatment of Parkinson’s disease (PD). An initial review of data from three separate Phase 3 trials did not provide evidence of efficacy for preladenant compared with placebos. Based on these results, Merck decided to discontinue the extension phases of these studies and no longer plans to pursue regulatory filings for preladenant. This drug was considered to the perhaps the most significant competitor for tozadenant, so its failure could be considered to be positive for Biotie.”
Personally, I don’t understand why two seeming failures of drugs targeting the same receptor would seem “positive for Biotie.” Wouldn’t theirs likely meet the same fate? Is there such a difference in these drugs seeking to use the same pathway? I know Biotie’s tozadenant had a positive review in The Lancet: http://www.thelancet.com/journals/laneur/article/PIIS1474-4422(14)70148-6/fulltext
and this is the basis for Biotie’s desire to advance tozadenant to Phase 3, for which they seek a partner.
As far as I can tell, neither of these analysts’ websites shows any recent news or opinions that might account for the downdraft in BIOZF. I’m down also, & haven’t sold. I notice that BIOZF has rebounded 3 cents (12%) so far today on what yahoo says is 5,900 shares traded.
Thanks for digging all that up. I used translation software on the Inderes site. The scientific case for tozadenant was made in my column. Both analysts have completed ignored what I regard as the company’s best assets: nepicastat and the VAP-1 monoclonal.
Nepicastat impresses me mechanistically and because I just tend not to regard any other drug therapy as working for cocaine addiction, I have treated many cases of it…..it is VERY difficult to treat. An agent with any promise would excite.
PSC is an off-the-beaten path illness, but I will ask people to take in on faith from me: orphan or not, if the phase 2 is positive, this will cause a rumble in shares. People need to understand how deadly and futile this disease is, how we have nothing for it. Breaking the news of a PSC diagnosis to a patient has caused me to cry before, because it is horrible in so many dimensions. If the antibody works in phase 2, someone will come in and partner with them for phase 3.
I feel that both the Edison and Inderes reviews, both of which I gave links to in my column, are while fair, also tepid and lacking in any measure of enthusiasm. I’m not sure they have talked to the CEO. I have, and I like him and i have confidence in him. He is fired up. To my mind, their neurology drugs are the least interesting thing they have. However, their adenosine receptor acting agent is in a different class, acting in a different way. The Japanese drug is scientifically pretty weak, I feel.
As always, Dr. KSS, many thanks for your insightful reply and all you do here to keep us gummies so well informed.
You’re right, the two analyst houses place most of the value on Selincro & tozadenant. Your preference for Biotie’s lesser-known assets helps me also feel that this is one undervalued stock.
Thanks, life. When I talked to Veromaa, the CEO, I tried to really pump him up about chasing PSC, as they have mainly been a neurology company. He is no wallflower, and believe me, he gets it. It is good for shareholders when the CEO has itchy feet! Selincro will never bust blocks, of course, but it is a steady source of some income, and some profits. Unfortunately, because of patent deficiencies they can’t pursue it in the US. But keep in mind this: that the markets in which Biotie has yet to roll out Selincro are, in combo, bigger than all the markets that now have it. And keep in mind its mech of action: it helps people cut drinking over a long period of time. This is better than the sudden-stop approaches because of the nature of alcohol’s action on the brain. If you take 3 Xanax a day for 5 years and then suddenly stop, guess what: you are going to go bonkers and you may seize. Things must be tapered. It is not about willpower. This cuts the cravings and the pleasure of drinking. But honestly, given my view of neurology, and given how rarely neuro trials pan out well (the stakes in Alzheimer’s are appalling…chance of success approx zero)…if I were just zeroed in on the neuro portfolio at Biotie as these 2 analysts are, I’d be bored stiff too.
I have been treating PSC for almost 20 years, speaking on it, writing on it, and have never seen anything within a light year as promising for it as Biotie’ s antibody. The science is just so compelling. Biotie just sits there ignored, because people don’t think of Finland when they think of biotech, and because the EU’s analysts do not cut and carve and dissect these companies as effectively as the Americans do.
I overlooked something interesting in Biotie’s news releases June 30th & July 30th, indicating that they are preparing to run the tozadenant phase 3 trial by themselves. They consider it to be their most valuable asset; maybe they should check with you, Doc. I quote:
“Following the decision by UCB Pharma S.A. to return global rights to tozadenant in March 2014, Biotie has been evaluating the most suitable development strategy for this Phase 3 ready asset to maximize its value to shareholders and has concluded that this can be best achieved by continuing with the Phase 3 study within its current portfolio. The Company considers tozadenant to potentially be its most valuable asset given the high unmet medical need in Parkinson’s disease and stage of development and is currently evaluating various options, which may include a capital increase, to support the clinical studies and a strong regulatory filing package for tozadenant.”
I don’t think it originally sunk in with me that “within its current portfolio” means run the trial on its own. They’ll also freeze their SYN-120 phase 2 testing in Alzheimer’s, which as you indicated above, is probably a good idea based on chance of success.
I google translated the July 31st reaction by the Inderes Oy analyst Juha Kinnunen (a translation is an awkward thing to read; btw, “Biotie” translates to “Life”) in which he seems surprised by this choice to go it alone rather than partnering. He says Inderes previously estimated the cost of a P3 at 100 million euro, but now thinks it can be done for around 80M. Says the company may raise funds by debt issuance, share issuance (current number of registered shares: 456,032,398), sale of rights, or sale of product portfolio, and speculates that they would sell their VAP-1 agent & nepicastat, if successful, to help fund the toza phase 3. Plus use Selincro’s future profits…or…(c.y.a.)…find some other way. I s’pose the options are fluid at all times with small biotechs. Another interesting thing is that at the time of Inderes’ April Initial Report on Biotie, its shares were at .22 euros (now .19) and their target price was .32 euros. Seems like here in the states we hope for a larger gain. Maybe we’re greedy. I’M sure hoping for more than a 10 cent profit.
Thanks sharing that Biotie piece, pie!
No schadenfreude meant, but $GILD longs rejoice.
BMY (Bristol Myers) phase 3 trial in gt 1 HCV just suspended on safety concerns.
Shouldn’t the I in $GILD be changed to an O?
Insider trade: DRTX officer purchased 3,000 shares @ 13.72.
http://content.stockpr.com/sec/0001209191-14-052202/0001209191-14-052202.pdf
$DRTX’s chief commercial officer just grabbed 3000 shares.
Doc KSS,I am with you on the Biotie CEO and thank you for bringing this company to our attention. I bought in last week and was concerned about price drop and volume.He emailed me back promptly and quite frankly I am very fired up about this company and will add more.Like you say Doc, this guy seems like a leader and someone you want your money invested with.Here is what he had to say.
Dear Glenn,
We are on track with our development plans with a flurry of positive news over the past couple of weeks:
We have announced non-dilutive financing for SYN120 from The Michael J. Fox Foundation to do a Phase 2 study in Parkinson’s dementia, we announced grant funding from the UK government for BTT-1023 for a Phase 2 trial in Primary Sclerosing Cholangitis and we continue to have full support from the US taxpayers where NIDA is funding and conducting a phase 2 study in treatment seeking cocaine addicts with nepicastat. Topline data is expected at around year end.
For the lead development program, tozadenant for Parkinson’s patients suffering from motor fluctuations, we announced publication of the robustly positive clinical trial results in the leading clinical neurology journal, Lancet Neurology and we are in full swing to get the Phase 3 trial started H1 2015. We and the FDA consider the now published study to be the other pivotal study and are preparing to repeat this already successful study and then submit an NDA in the US.
Selincro, our alcohol dependence product marketed by Lundbeck, received a significant vote of confidence from the UK Health Economics Authority NICE when in July they published a very positive assessment essentially stating that Selincro is good value for money and that it should be included in the NHS reimbursed prescription medication. We expect Selincro to bring in six million euros in launch milestones and the beginning of a royalty stream which in due course we expect to grow significantly. Lundbeck is forecasting the peak sales of Selincro to be USD500 miliion per annum but it is still early days and we expect Selincro to be a solid revenue generator for Biotie in the years to come.
The financial situation of the company is stable with EUR 34 million in cash.
It seems that the markets are not appreciating all these positive developments but we are working hard to spread the positive news and explaining to institutions our strategy and intentions to bring tozadenant to the market on our own.
Happy to talk over the phone should you wish to discuss further.
Best regards,
–Timo
Timo Veromaa, M.D., Ph.D.
President and Chief Executive Officer
Biotie Therapies Corp.
Joukahaisenkatu 6
20520 Turku
Finland
+358 2274 8901 (Direct)
+358 2274 8973 (Executive Assistant)
+358 40 5739933 (EU Mobile)
+1 650 445 8314 (US Mobile)
timo.veromaa@biotie.com
http://www.biotie.com
This email message is for the sole use of the intended recipient(s) and may contain confidential and privileged information. Any unauthorized review, use, disclosure or distribution is prohibited. If you are not the intended recipient, please contact the sender by reply email and destroy all copies of the original message. If you are the intended recipient, please be advised that the content of this message is subject to access, review and disclosure by the sender’s Email System Administrator.
Please consider your environmental responsibility before printing this e-mail
—–Original Message—–
From: glenn newberry [mailto:newby3867@yahoo.com]
Sent: 13. elokuuta 2014 6:36
To: Timo Veromaa
Subject: Shareholder
Tim,excited about your company and invested in it.I am a little concerned over the high volume of shares being traded recently to the negative side and losing about 40% for the year.Just would like some reassurance that company is on track with their goals going forward.Long Biotie and thanks in advance.
Cheers,Glenn Newberry
Good job Glenn and good info. And did I notice that the president/CEO is an MD and PhD , unlike ……….
MD PhD’s rock!
He may not be an MD., Ph.D., but he is a Ph.D., MD.
http://www.benitec.com/management.php
Means managing director. No MDs in Australia (MBBCh)
Thanks Kenny,and thanks for what you do here as well.
Cheers,Glenn
Very intrigued by Biotie but do we know why their partner relinquished their global distribution rights for the Parkinson’s drug? They presumably know the Phase 2b results.
Read the column by me on Biotie, This was explained there, and as I discussed there is not a cause for concern.
Got it; thank you for your response
Glenn: one hugely helpful tidbit in what Veromaa said: the phase 2 tozadenant study that appeared in print will count as pivotal for FDA approval. The FDA wants two studies. this means they will only need to do one more, not two more. Very good for them! It’s news….they gave clearly met with the FDA recently.
Very good news indeed Doc.Things look sweet for Biotie for the future.
Cheers,Glenn
This article should bode well for some of the antibiotic stocks we are involved with here for the future. http://www.news-medical.net/news/20140813/MRSA-and-antibiotic-resistance-is-a-major-health-threat.aspx
Cheers,Glenn
Hi Lawrence McKenna; a tip for those long URL’s in your post #240 above. Go to the TinyURL website and copy the link to your bookmarks bar (after Apps). Then all you have to do when you have the subject website in view, is click on TinyURL and click on clipboard. I just did and here it is;
http://tinyurl.com/mtdnrwo
We’ve not run the list in a while. Based on what I know
AKAO buy/long
ALKS buy/long
ATHJF hold/long
BIOC buy/long
BIOZF buy/long
BTEBY hold/long
CBST hold/long
CTIX buy/long
CELG buy/long
DRTX buy/long
ESPR buy/long
FOLD buy/long
GILD buy/long
ISRG hold/long
OXBT hold/long
PTN hold/long
RGDO buy/long
SNWV buy/long
SVA buy/long
NVO buy/long
TMO buy/long
Dr KSS: I’m sorry…think CLDN (CELLADON) is one too. Have a blessed week!
Guess you have CLDN at buy/long
Yes, sorry I missed that one. Now is an rare optimal entry point too.
Dr.KSS: Are you sure about Cubist on the list? In post 160 you seemed to be down, putting it mildly, on the company.
Perhaps relatively down, but not elementally against it. I wouldn’t buy here but will be holding all my shares. It has scored many accomplishments this year, but its next milestone is unclear. I try to air all concerns and discuss things here so people can be informed, make good decisions. The company is transitioning into being now a profitable one that will be denominated and judged by different criteria. I feel it’s reasonable to be long on a company but also have, and air, concerns. They need to get QC up to speed. I wish they’d snap up $DRTX. $DRTX in its present form, with one drug and a whole company built around that, is somehow to me like free GSH glutathione in a cell…something is going to react with it. $DRTX will acquire something or be acquired. Same cannot be said for $MDCO (oritavancin).
Also, long Elliot’s JNJ, I looked into the pipeline….very plump and juicy.
LOL thanks for the plug, doc. I think JNJ is best of breed of the dinosaurs in the healthcare/pharma sector, and I like their prospects. It won’t be a huge gainer, but with compounded dividends (which they are always raising) and steady growth over the years, this is a solid stock to sit on for decades. It’s important to have some conservative picks, no matter how bullish you are on the little guys and the tiny guys … the fact of the matter is that some of them (and likely most of them) will fail. The hope is that a couple of massive winners will outshine the losers, but in the meantime, it is good to have some safe money.
That said, I think GILD is a better safe pick right now, and I will add to GILD on a pullback faster than I will add to JNJ on a pullback. I think GILD is due to rocket higher … just hoping I will get one last chance to add.
Elliot,
I own some J&J thru Scotttrade but understand they have a drip plan where you can make monthly investments without paying trading fees. Just wondering if you’re familiar with it and whether you purchase your shares that way or not.
I’ve heard of DRIP plans, but I am not currently enrolled in any. I currently use Scottrade’s FRIP plan, where I am free to invest my dividends into several different companies and I don’t pay transaction fees. I like this plan currently, although I hear some DRIPs offer a reduced price at which to reinvest.
Very few DRIPs offer discounts these days, though a few do. They can often be cheaper than even a discount broker for the very small regular buyer (ie, buying $100 worth a month), partly because you can buy partial shares, but in many cases investors who have discount brokerage accounts that will reinvest dividends for free get essentially the same thing and sometimes at a lower fee. JNJ does not offer a discount in their DRIP, FYI, and they do charge a fee — though it’s much lower than most brokers at $1 per recurring buy (sales are a bit more expensive than most brokers, but these aren’t plans where you trade in and out — details for JNJ at https://www-us.computershare.com/investor/3x/plans/planslist.asp?planid=290&state=eStateDisplayPlanSummary)
Thanks, Travis. I do know that Silver Wheaton (SLW) recently initiated a DRIP which includes a discount that I believe is somewhere around 1 or 2% less than market price. I did not know this was uncommon.
Interesting, hadn’t noticed that — I love dividend reinvestment, though it’s a balancing act of fees and convenience and recordkeeping (and sometimes discounts) to decide whether to do it directly or let your broker do it for you. Sometimes the direct DRIPs are a better bet for investors who are their own worst enemy (as is the case with most of us who trade too often), because they are separate and easier to set aside and ignore while they compound, with less temptation to sell them so you can buy the next “hot” idea.
Travis, Sharebuilder.com will reinvest all dividends at no charge and all other transactions, buying or selling are 6.95.
That’s slightly cheaper than most … Don’t they also have cheaper recurring/automatic trades? The cheapest broker I’ve used recently is interactive brokers,
But they don’t have the handy reinvestment or automated stuff.