Robert Morris is helming a biotech-focused stock newsletter that’s called Biotech Supertrader (modesty has no place in the world of newsletter promotions, of course), and I’ve never covered this letter before so I thought I ought to have a look at the latest teaser we’ve been asked about.
Morris, incidentally, has been featured in our pages before — but that was back when he was editor of China Stock Insider at the same publisher. That letter, like almost all China-focused investment newsletters, seems to have disappeared quietly into that good night … which probably tells you that it’s time to invest in China again, since the newsletter publishers are ignoring the Middle Kingdom and rushing out their pitches about biotech and tech stocks. At the time, Morris was teasing NQ Mobile (NQ), which has turned out to be pretty good if you bought it down there in the $6-8 neighborhood (though it’s been a wild ride).
So now what’s he pitching for his Biotech Supertrader?
Well, the destruction of “Man’s deadliest disease”, of course. Here’s how the teaser gets our attention:
“This Tiny, Unknown Biotech is About to Unleash Its ‘Holy Grail’ Drug on Man’s Deadliest Disease
“Their ‘Guided Missile Approach’ Could Save Thousands of Lives Each Year
“It’s about to become the most talked about advancement in cancer treatment in our lifetimes and you can lock in a life-transforming fortune if you act quickly….
“I’m urging my subscribers to load up on this stock NOW….
“I’ve just uncovered a tiny, unknown biotechnology company with a new cancer drug in phase 3 clinical trials which is showing remarkable success at treating several types of cancer.
“Their scientists have found an innovative approach to cancer care which involves a breakthrough in treatment. It goes deep inside the inner workings of our cells.
“Plus, this medicine looks to be many times more effective and with fewer side effects than the chemo, radiation, and drug therapies currently available.”
If there’s one thing that investors know can make them rich and make them feel good about themselves and the world, it’s a cure for cancer — we’ve seen that effective cancer treatments can and do (occasionally) turn little biotech stocks into gigantic successes, so the dream lives on that you’re going to catch one of these lottery tickets and own the next Genentech. Will we be so lucky? Well, let’s see which one he’s pitching:
“When this drug wins FDA approval – which I believe it will – this small company’s $4.16 stock price will go straight to the moon.
“And the market for this drug is absolutely huge!
“You see, this small biotech is targeting its new drug, let’s call it ‘drug S’, at cancers of the blood and bone marrow. And it is already in very promising phase 3 trials for these two types of cancer.
“But here’s where it gets really interesting. It looks like the drug this company is developing will also work on other types of cancer!
“There are positive signs it works on Non-Small Cell Lung Cancer (NSCLC) too. There are 1.1 million people with this type of malignancy. Just in the United States alone there are over 300,000 patients with this disease according to The American Cancer Society. Each desperate for a cure.
“Plus it looks like ‘drug S’ may turn out to be an effective treatment for ovarian Cancer. There are more than 204,000 new cases of ovarian cancer diagnosed worldwide each year with 22,280 of these in the United States according to the National Cancer Institute estimates.”
So … who is it? Thinkolator sez this is Cyclacel Pharmaceuticals (CYCC)
Cyclacel is indeed a little biotech around $4 (it closed at $4.35 yesterday), with a market capitalization of only about $80 million — so be careful, we’re a big enough group here that if just a small percentage of Stock Gumshoe readers got enthused about this stock it could drive the shares up, less than a million dollars worth of shares trade each day (Biotech Supertrader says they limited their readership to 750 people — I don’t know if that’s still their cap or if they’ve hit it, but we’ll have more folks than that reading this free article).
And like many biotech stocks, it’s got some impressive scientists and it’s been losing money for a long time as they’ve been searching for a viable drug (their current lead drug also was a big focus of theirs back when it was in Phase 1 trials five or more years ago, so that’s a good reminder of the time these things take, it’s just starting Phase 3 trials now). It looks like they must have gone public in 2004, when they were about eight years old, and a quick scan of ten years of their financials over at Morningstar indicates that they’ve never generated more than a token amount of revenue (meaning, they’ve probably had some research collaboration payments or partnership funding, but never got a product to market), and have accumulated more than $250 million in losses to date. And had two reverse splits to keep the price from sinking far into penny territory.
So that’s not unusual, but it means that — as with all developmental-stage biotechs — it’s not about the financials or the fundamentals, it’s about what’s going to happen in their clinical trials and whether things are going well enough that they can continue to finance the trials … which get much more expensive as you progress through Phase 2 and Phase 3.
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All I know about them so far is that they say they’ve got enough cash to get through enrollment in their key Phase 3 study for “drug S” (which is sapacitabine) as of September when they last updated their investor presentation, but I know nothing about the science or the competing cancer drugs that are out there or how fabulous this particular one might be, so I asked our favorite medical writer, Doc Gumshoe (who, yes, is not a doctor) to check them out quickly and chime in. Here’s what he could share after looking into them for a few minutes (he’s just looking at the medical stuff, not so much the “investor presentations”):
- Cyclacel’s Prospects
Cyclacel has three drugs in development at this time, and is involved in eight clinical trials with these drugs, not including two clinical trials that have been terminated. Their top contender is sapacitabine which targets the division of cancer cells. If you can prevent cancer cells from dividing and reproducing, you have the cancer whipped, so targeting cancer cell division (or mitosis, which is the technical term) is a highly promising avenue for treating cancer. However, we need to take note of the fact that sapacitabine is one of a large number of drugs that propose to fight cancer by this method.
At present, all eight of Cyclacel’s clinical trials involve sapacitabine. Of these, at least one has been completed – a Phase 1 study of the safety and pharmacology of the drug. Four others are current, with no information about results. These are likely Phase 1 or small Phase 2 studies, to assess safety, determine what a correct dose might be, and evaluate whether the drug does what it’s supposed to do in human subjects with the target diseases, which in this case include acute myeloid leukemia (AML), cutaneous T-cell lymphoma, and some advanced solid tumors. Prior to the clinical trials, sapacitabine has demonstrated impressive results in delaying the spread of metastatic liver cancers in mice.
From what I can gather from public sources (i.e., the NIH Clinical Trials Registry), there is one Phase 3 trial, which started recruiting patients in February of 2013 and is expected to be completed in late 2015. The trial is in elderly patients with AML, and compares alternating cycles of sapacitabine and decitabine with decitabine alone. Decitabine (Dacogen) is FDA-approved for treating AML and also targets cancer cells’ replication by attacking their DNA.
It is possible that the Phase 3 trial by itself could lead to FDA approval for sapacitabine, depending on the strength of the results. However, that trial would not get the drug approved for use as monotherapy, since it is not being investigated as monotherapy. My guess is that Cyclacel is planning more trials of sapacitabine as monotherapy, perhaps in younger patients. And my further guess is that FDA approval is still quite a long way off.
Sapacitabine is also in a Phase 3 trial with cyclophosphamide and rituximab for the treatment of relapsed chronic lymphocytic leukemia. Cyclophosphamide (marketed under several trade names) is a well-established chemotherapy agent used in a number of cancers, and has led to remission in many cases; however, it is associated with truly harrowing adverse effects. Rituximab (Rituxan, Genentech) is used not only in cancers but in some autoimmune diseases. And sapacitabine is also being studied in patients with previously-treated non-small-cell lung cancers.
Although the piece from Biotech Supertrader said that the drug – identified as “drug S” –is also a promising treatment for ovarian cancer, I find no clue that it is being studied in such patients. [ed note: that’s because that “promise” is in the lab still, not in people — they had a press release about this in the Fall, “75% of Ovarian Cancer Patient Samples Highly Sensitive to Sapacitabine”, not studied in patients but on patient samples]
Cyclacel has two other drugs in development: selicilib and a drug designated as CYC116. One selicilib study has been terminated, and in a second Phase 1 study, selicilib is used with sapacitabine in patients with advanced solid tumors. Remember, however, that Phase 1 studies are many rungs of the ladder below what’s needed to gain FDA approval.
CYC116 is an aurora kinase inhibitor, meaning that it blocks the action of an intracellular enzyme that facilitates cancer cell mitosis. This is a promising avenue of cancer treatment, however, the traffic on this avenue is fairly heavy, and includes several other classes of drugs including tyrosine kinase inhibitors, and taxol based agents such as paclitaxel (Taxol, Bristol Myers Squibb); docetaxel (Taxotere, Sanofi-Aventis), Abraxane (a newer formulation of paclitaxel from Celgene) and others.
CYC116 supposedly also inhibits vascular endothelial growth factor (VEGF), which induces the growth of blood vessels that nourish cancer cells. Inhibiting VEGF is a well-established means of combating cancer, and CYC116 could hardly be characterized as a radically new departure in cancer treatment.
The one trial involving this agent has been terminated. That, of course, does not mean that development of CYC116 stops dead in its tracks – there are many reasons why a trial can be terminated, and ours is not to speculate without more information.
Beyond those three drugs, it’s hard to guess what Cyclacel may have up its corporate sleeve. It is certainly true that a successful cancer drug – even if only moderately successful– can be transformational for the biotech that develops the drug. But the drugs that Cyclacel has under development do not appear to this skeptical observer to be radically new departures in cancer treatment.
It’s important to remember, when trying to estimate the likelihood of a single drug demonstrating sufficient efficacy and safety to gain FDA approval and market share, that the competitive field is vast. As I mentioned earlier, Cyclacel has a total of 8 clinical trials in process at this time.
For the sake of perspective, it’s worth knowing that at present there are 41,445 cancer trials being conducted. So those are the odds.
So there you have it — it’s almost impossible to find a development-stage biotech whose financials look great or that makes your heart go pit-a-pat over their valuation, especially in a biotech bull market like we’ve seen over the past year or so, and Cyclacel doesn’t jump out as spectacular on that front either, not unless you’re a big believer in the promise of their specific drug. They’re a small stock and they don’t get much attention, other than from the analysts who probably helped them sell shares in secondary offerings in recent years, and there aren’t any major “skin in the game” insiders as far as I can tell (the CEO owns $1 million worth of shares, but he gets paid more than that every year), and there’s only one really focused owner on the institutional side that seems to have any kind of biotech focus (Eastern Capital owns about 7% of the shares, roughly $5 million worth … don’t know much about them).
So I don’t see a lot to make them stand out other than Robert Morris’ apparent enthusiasm for the shares (which certainly goes over the top, he calls his special report “The End of Cancer Worries Forever“), and I don’t know enough about the science to be a believer (though, to be fair, I almost never speculate on developmental biotechs because they’re so hit-driven and I’m not smart enough to be a hit-picker in the sector). It is at least encouraging that they are enrolling patients for Phase 3, and that they probably won’t have to raise more money before they have some indication of how the trial is going, but sometime in the next year or two they’re probably going to have to either get good results from this trial that let them raise cash at a good price, or have promising enough results that some big pharma company wants to jump in and help fund development of “drug S” (or just buy up the whole company, as happens with some regularity when a little biotech gets promising results).
Oh, and they are presenting at an investor conference next week, so maybe they’ll have something interesting to share then. As you can tell, this one doesn’t jump into my cup of tea … but these kinds of stocks almost never do. Sound interesting to you? Interested in the science or the lottery-ticket possibilities of $80-million developmental biotechs? Have any experience with Robert Morris or know whether or not we should consider him a biotech savant? Let us know with a comment below.
Well…. today should be an interesting day for BNIKF after last nights action in Australia. While that plays out today, I just wanted to pass along the latest info for those interested in INO (Inovio Pharma). Just as the stock reached a new all time high last week, they went out with an offering to raise $63M even though they claimed to not be strapped for cash. The CEO of INO had an interview with a SA author to explain the company’s logic. Being a long term holder of INO (cost basis 0.82) I was concerned about the stocks dilution and subsequent price drop-off. After reading Dr. Kims explanation I am not as concerned.
http://seekingalpha.com/article/2070113-inovio-pharmaceuticals-raises-63-million-dr-j-joseph-kim-ceo-tells-us-why?source=yahoo
PPHM is going nuts guys … any thoughts on this? Technical analysis? I know earnings is tomorrow, but why would an unprofitable biotech stock run up into earnings? I guess I seem to remember maybe they already have a product that is in the market. Idk my mind is so jumbled from trying to follow so many (haven’t been successful on a single one yet, hoping MNKD changes that).
OK so they do have revenues. Maybe there are thoughts that they will be profitable this quarter
Added 5k shares @1.75. If it dips i will add more. No good reason for the sell off in Aussie land.
Anyone got any thoughts on CVM? Looks ready to make a possible run.
Dr KSS … Do you have any thoughts on the combined HIV and hcv treatment that Biotron BIT released today that knocked the stuffing out of BLTs share price in Oz?
http://seekingalpha.com/article/2087783-cel-scis-multikine-potential-21st-century-superdrug
Biotron also received a patent in the US covering BIT225.
From their website: “Biotron’s lead drug, BIT225, is a viroporin inhibitor in clinical development for treatment of HCV and HIV, as well as the hard to treat HIV/HCV co-infected population. It has shown good anti-HCV activity in clinical trials to date, improving the outcome in patients with hard-to-treat genotype 1 HCV infection undergoing treatment with current approved therapy of interferon and ribavirin (100% receiving BIT225 (400mg) plus IFN/RBV were virus-free at 48 weeks, compared to 75% who received only IFN/RBV).”
Hopefully, the good Dr. will comment.
FWIW: Their treatment is 12 weeks long as opposed to BLT’s one shot and you are done.
Dr KSS: Any thoughts on Biotron (symbol = BITRF:Grey Market)? Is this a company worth putting a little speculative investment into with hopes of knocking one out of the park or is it too risky given the stock is on the grey markets? Any insight into the company would be appreciated!
http://hcvdrugs.com/ BITRF and BLT both are listed
To David Belan: I have been bird-dogging Biotron since late last night when I got word that shares were soaring. It does trade here but seems to do so in a very illiquid manner, though that may change.
Their drug candidate is an inhibitor of p7, an HCV viroporin. HCV gets into a cell, makes new copies of itself, packages those, and then those must get out of the cell to infect other cells. Packaged virions escape either by killing the cell, or in the case of HCV, by p7 assembling itself into a porin, or membrane channel, a conduit out of the hepatocyte.
In my view, the press release that sent these shares rocketing was a scientific nonevent, though one that shows they know how to do good PR. In a small phase II study, they took HIV/HCV patients whose HCV genotype was 3, and gave them either PEG-IFN/ribavirin, or PEG-IFN/ribavirin plus the p7 inhibitor. The press release was that those patients are still sustained virologic responders at week 24. This is a non-event because they were SVR at week 12. If you are SVR-12, you will be SVR-24 invariably. In their study, 75 per cent who got IFN/ribavirin were SVR (a typical percentage for genotype 3). 100 per cent who got IFN/RBV plus p7 blocker were SVR. This is good. The drug may well take its place in the armamentarium for HCV in combo with others. It will not be usable as monotherapy.
This company may very much have the drop on this class of viricidals, as I know of nobody else pursuing these. The viroporins have been known about for perhaps 12-15 years, but have thus far not been drug development targets that I know about.
This company will have to raise capital like mad to get this to market, and they need to do more HIV studies as they allege it has anti-HIV activity. I messaged my brokerage firm last night to find out why the shares seem rarely to trade here. It may be from the company being unknown, lack of interest. I suspect that will change. I am trying to find out who the market-maker is.
The Biotron event has moved BNIKF’s RSI finally to less than 70, which makes for a good time to get in. This company poses no threat of any kind to Benitec. Different field, different aims, no competition. I bought more Benitec today. To me it looks cheap again.
Thanks Dr KSS
http://www.benitec.com/documents/140106_Qantas_Bright_Ideas.pdf
All of the action in ARWR is just unseemly! OK, they got clearance to give their siRNA drug to Hong Kongers with chronic HBV. I see a couple of problems here. One, those patient will get one or two doses of drug. Nothing more. This will of course not cure HBV. They are looking for degree of response in terms of decrement in HBV surface antigen and DNA. But they are not going for cure. One or two doses will not cure. Patient may need 6-12 months of therapy. They also chose HBV E antigen negatives, which is strange to me. Those patients might shine more on treatment. Finally, I recently posted here an article about using ddRNAi to kill HIV. Basically the message of that article is that if you use one or two strands of RNAi, you get problems with virus escape mutations. When you use three bits of siRNA, you keep escape mutation down to a manageable nil level. ARWR is only using two strands of siRNA. Benitec’s genius with TT-034 is going after three targets at once, basically so that they nix resistance mutations and virus breakthrough. People just do not realize how far ARWR has to go on this.
People should really see this article, as increasingly this consideration (a company’s ZIP code) is figuring into my thinking when I look at biotech:
http://www.fiercebiotech.com/story/top-15-cities-biotech-venture-funding/2014-03-06?utm_medium=nl&utm_source=internal#anchor
RE-BNIKF, There is an article today in the NEJM about CCR5 suppression in HIV patients . Autolagous cells were modified using the “zinc finger” method. They appear to have had some success. The study was apparently done by Penn State and “Sangamo Bioscience”.
PS- It was not the Calimmune study that uses Benitek technology. We are still waiting for HIV results for that as I understand.
To Larry Wright: Thanks for pointing that out. Overall I don’t think Sangamo’s method is as persuasive as what Benitec’s will afford (its ddRNAi is licensed to Calimmune for this purpose). Calimmune is taking a lentiviral vector and adding to its genome shRNA to go after CCR5 as well as a gene that encodes an HCV fusion inhibitor. They plan to put this into trials first in AIDS patients to see if it allows them to come off ART drugs. I suspect it will. I do so wish Calimmune was publicly traded. It will be eventually, But I am less keen on Sangamo than I am Cali and Beni for this clinical problem.
Thanks- My PS and your response crossed in the mail.
That’s what I was hoping, but it seemed very close. They had very few patients and their primary endpoint was safety, but reported some efficacy data.
One more thought. A comparison of Sangamo and BNIKF is interesting. Their lead product, the one reported, is in phase 2 at about the same stage as Benetik’s. They are aiming at HIV, B is aiming at HCV, with crossover application including Calimmune’s HIV trial. S went up 23% today with this announcement. THEY HAVE A 1.5 BILLION market cap.
This confirms, again in my opinion, your analysis of the potential room for appreciation for B. The only real surface differences between the two seem to be they are a California co. and are NASDAQ listed. Therefore I, like you , loaded up some more B.
FYI, i put a bid in for 10K shares of BITRF about 12 minutes to close, and it did not get executed.
i have to wait to the next day to see if my order got through (europe) or stay up all night, lots of lost connections with australia. Maybe bad broker.
Good points Larry. As I see it, Benitec’s TT-034 trial is really a study with outcomes on 2 fronts. One question to be answered is: does ddRNAi work in people? Except for Calimmune studies looking at subtherapeutic dosing in HIV patients, we do not know. Much will ride on what happens with the first patient, who has probably been dosed this week. When that patient undergoes liver biopsy in a few weeks, tissue will be FedEx’d to Sydney for in situ hybridization studies looking at whether that patient’s liver cells are actually cranking out shRNA.
The second outcome is whether an approach that silences RNA from three parts of HCV genome actually conquers HCV.
The study could succeed on either prong, or on both. They are separate. BUT if it succeeds on either prong, shares will go up like mad. If the study succeeds in both ways: high liver transduction, as well as suppression of HCV virus in blood, expect a party like it’s 1999. It honestly could go from being a $150 million company to be a billion dollar company if that happens.
I know they have the ability to release findings on an interim basis. I also know you have communicated directly with them. As a practical matter, what do you think is a reasonable time spectrum to expect news on the results? Is it the same if favorable or no?
Hi Karma, from my understanding, the Calimmune trial is a PI/II with the cohorts receiving either Cal-1 alone, or Cal-1 with either a low-dose Busulfan, or a med-dose Busulfan. I thought that the clinical trail included a therapeutic dose but perhaps you have more information than I do. Could you confirm?
Larry: I must say I do not know. My prediction is that they WILL want to release interim data, because they will miss the EASL meeting but AASLD is not til year end. If they release data, they drive up share price, which they need to do so that they get better terms when they have to raise capital again.
I need to review the dosing cohorts for TT-034, but as I recall, patient zero gets dosed and assessed for six weeks before the next patient is dosed. Both those first two patients will get what are thought to be subtherapeutic doses, just so it is not Jesse Gelsinger Redux. If I were at the company, I would NOT release data on one patient, because it means nothing. Anything can happen with one patient. But once they have data on two patients, and if those data are congruent with each other, that becomes a news item. Realistically that is end of May at the earliest. But my sense is that now that they have skin in the game, and understand markets, they are not going to wait til winter 2014 to release the first TT-034 data. That’s too long in biotech land.
KarmaSS what do you think of neuronal nicotinic receptors? Here’s a beaten down biotech company left for dead by many in the Fall of 2011 when their lead compound, an antidepressant, failed in trials. The company is Targacept Biotech out of North Carilina.
What intrigues me is that they have 4 compounds in Phase 2 currently and $144 million in cash with a market cap of $165 million. Add to this that they have 75% institutional ownership and that BlackRock took a big stake on Jan. 30th now owning 7.2% of the shares, I am intrigued. The current market cap indicates that the 4 compounds are virtually worthless given that it is about even with the cash on hand.
Either this is a truly worthless company, or it is a great bargain right now, espc. if any of its compounds holds decent promise. The fact that BlackRock just took a big stake really intrigues me. What do others think?
To David B: Do you know anything more about the agents Targacept is trialling? You are right, they have been left for dead though they are a very smart company. I believe it was their work that led to varenicline, Chantix, though that drug has had serious concerns raised about it (homicides and suicides on it).
Here is my take on tobacco and nicotine. It may shock you, but I love a good cigar now and again (there is a cult among GI doctors as regards cigars). But I can go for months without them and never miss the nicotine, despite the fact that they have at least 70 times more of it than cigarettes. In fact, nicotine is, mg per mg, 70,000 times more habit forming than cocaine. There is a reason for that, and I think it is the reason I do not miss nicotine: nicotine is, in most people, very rapidly metabolized. And this is the secret to an agent being addicting: it must be fast on, really have a strong psychotropic effect, BUT also be fast off. By testing, I have unusual genes: I am one of 15-20 per cent of people who has a defective liver allele for the cytochrome P450 enzyme that breaks down nicotine. Thus if I have a cigar, that nicotine disappears from me very very slowly. I don’t miss it. But most people are left craving it a few minutes later. And I have felt that poisoning that P450 in normals could be the great cure for tobacco dependence.
This slowness versus fastness in breakdown is why doctors are terrified of prescribing, say, Xanax, versus Valium. Valium has a half life of 96 hours, which makes it much harder to get hooked on. Xanax, however, disappears very very quickly, and 50 per cent of people prescribed it are hooked by the second prescription (I have never prescribed Xanax and never will.)
NNRs contribute to a wide range of brain activities and influence a number of physiological functions, and in recent years it has been discovered that they are present in a number of non-neuronal cells where they play a significant functional role. It is believed, that in utilizing the right method of execution, that therapies such as the ones being employed at Targacept could eventually be game changing in conditions ranging from overactive bladder, to Alzheimer’s, to perhaps even drug addiction. The science is unquestionably credible. The question is whether or not Targacept will be the company to capitalize on it.
The company’s current pipeline is attempting to do just that. At this time Targacept has three compounds of note, which are presently active in trials with specific targets defined.
Karma: from an article today on SA which is well written and thorough:
TC-5214 is a compound designed to treat Overactive Bladder. TC-1734 is a compound targeting Alzheimer ‘s disease. TC-6499 is aimed at Diabetic Gastroparesis. Readers will also notice additional compounds listed, which appear to be partnered with AstraZeneca (AZN). That partnership is being dissolved, and will be referenced later in the article.
For the time being however, readers should focus on the three active compounds being pursued. Of those three, the principal concentration of this article is on TC-5214 for Overactive Bladder. While Alzheimer ‘s disease and Diabetic Gastroparesis are sizeable and noteworthy markets, certainly capable of being treated with NNR based therapeutics, they are also so largely unmet that the pathway to approval through the FDA is an ambiguous one. That uncertain, and constantly metamorphic process, is destined to create obstacles yet to be seen. However, in the case of Overactive Bladder, a growing 3 billion dollar market, the pathway to approval is more clearly defined.
All of that is quoted from an article from “the Behavioral Economist” on Seeking Alpha. He writes thorough articles with an eye toward finding companies with big upsides and limited downsides. Targacept looks worthy of a close look.
Some insider buying from Dr. French. If I’m reading this correctly it looks largely symbolic (9939 shares) possibly because of what happened yesterday.