Dendreon and Provenge - The FDA Advisory Panel Meeting
On Thursday, March 29 I attended an FDA Advisory Committee meeting to review, approve or disapprove a new cancer treatment by Dendreon called Provenge. This treatment, if approved, would be the first therapeutic vaccine for cancer to come to market - Provenge is targeted at advanced metastatic hormone refractory prostate cancer.
The room was packed, and the most nervous group of people were from Dendreon (DNDN), the company proposing the treatment for approval. The Dendreon folks were even more nervous than the terminally ill cancer patients in the room to testify.
This hearing made history in many ways as Provenge was approved, not just as the first of its kind of treatment, but also the first approval by the FDA for a drug that failed to meet its clinical endpoint to stated goals in trial.
The actual vote by the 17 panel members at the end of the long meeting was actually going against the company when a man whispered into the ear of the person running the meeting and the world (at least Dendreon's world) changed, as did the vote, and a few minutes later the ninth yes vote was cast, the media relations person standing next to me from Dendreon began to show tears and some of the patients in the room began to think they might get a shot at living a bit longer.
Sounds overly dramatic? It was actually far more exciting than this - and, if you remember Mike Brown from FEMA, the man who went to dinner while the people of New Orleans drowned, I think he has a new home - the FDA - or perhaps at Dendreon. I am just joking but the level of screw ups by the FDA and Dendreon during the meeting was shocking, given the potential consequences - for DNDN, a business and billion dollars in market cap, for hundreds of thousands of patients, the possibility of a longer life.
Some background first. Provenge is a treatment, not a drug - an infusion of a patient's own dendritic cells, activated at a Dendreon facility by treating it with Provenge, and these cells in turn stimulate T cells in a patient's own immune system. Provenge is the first therapeutic cancer vaccine to be evaluated by the FDA. This created a very high bar for approval but that was only part of the problem.
Much worse was the paucity of data - Dendreon submitted data from two trials that had only 144 patients. But it gets worse than that - the trials failed to reach their stated goal or what is called clinical endpoint, reduction in the progression of the disease. And even worse than that (c'mon, this is fun), one trial had different results for the secondary endpoint - survival - than the other.
And therein lies the reason for approval - people did live longer. A secondary endpoint for the trial that has been called, by the FDA, the "gold standard" for cancer trials. On average, 4.5 months - but some have been alive for years and one appeared with his grandchildren at the panel meeting. The other reason for approval -- there are no other real treatments - the one approved treatment extends life less than three months and is highly toxic with terrible side effects on already weakened patients, side effects so bad many patients eschew treatment.
A third reason for approval was the panel itself - Provenge falls under the purview of Center for Biologics Evaluation and Research and was reviewed by the Cellular, Tissue and Gene Therapies Advisory Committee. The real gatekeepers of cancer therapies reside at the FDA in something called CDER - the FDA Center for Drug Evaluation and Research. They approve virtually all non-biologic cancer drug, are hard nosed statisticians and the two people on the panel who mostly work with CDER were the most vociferous opponents of approval.
A fourth reason was the composition of the panel - the FDA was very fair and had, I believe, seven immunologists on the panel, and these folks were eager to see some sort of treatment get to market. They also understood how hard it is to measure exactly how Provenge works - technically, the company cannot measure the real impact on the immune system in a meaningful way except through the extended lives of patients. The CDER people found this appalling; the immunologist readily accepted this as part of the newness of the technology. This lack of data on the actual mechanism of action of Provenge became an important part of the panel discussion - but actually turned in the company's favor due to the presence of so many immunologists.
The last reason was the testimony of the patients - all, technically dying except the grandfather who came with two grandchildren from California. They were all dying at different paces; most of them limped; one begged for approval for a dying father so he could see his grandchildren make their Bar Mitzvah. It may sound like a bad "made for television" movie but it was not. A very old hand at this, and maybe the best FDA analyst and watcher, Ira Loss of Washington Analysis Group, said this was standard at the hearings and had no impact on the panelists. But he spends all his time at CDER panels - two panel members at this meeting spoke of the impact of this testimony on their vote.
Yes, the vote - but before I get to the vote, let me take a moment to skewer Dendreon management. They were awful, with the exception of a consulting physician with experience in clinical trials. I subscribe to several fairly technical services and one went so far as to provide a biography and the past committee experience of each member. They also said there would be a spirited debate on the lack of data on the mechanism of action and this could hurt Provenge's chances.
Well, Dendreon management must not subscribe because they were caught flat footed at this discussion and did not prepare for questioning in this area. They played right into the hands of FDA statisticians and never once confronted, in their slides or formal presentation, the core issue - due to the small trial size and mixed results, by historical standards the treatment did not work. Thy were just about dead in the water when their consulting physician took the opportunity to seize the discussion during a Q&A session, steer the panel back to this issue, say Provenge worked and, politely explained that the patients were going to die anyway, what is the harm?
And that question - what is the harm - paved the way for the final, successful vote, sort of. Oh, before I get to that, let me tell you what your tax dollars buy you at the FDA.
Subscribes to my newsletter, ChangeWave Biotech Investor, besides having made an incredible pile of money on DNDN stock on Friday (I recommended the company in November of 2005) you would come to know I believe the FDA is the most undervalued, overworked and unappreciated of all government agencies --they need their own TV show, I guess, to get more attention from Congress. Their employees make one half to one quarter of what they could in the private sector and lobbying by Big Pharma, resulting in Congressional idiocy, has crippled them. For example, it now takes longer to get a generic drug approve din the US than a new drug because Big Pharma has convinced Congress to restrict funding for the staff that reviews generics. I estimate a twenty five million dollar increase in staffing would save Medicare and the Veterans Administration between $1.5 and $2.0 BILLION dollars a year.
Well, you get what you pay for - two leading figures in the discussion, senior biostatisticians who run divisions at the FDA, could not understand spoken English well enough to present proper testimony or answer questions adequately. They both had PhDs made in America but could not answer questions about the drugs they were evaluating, also made in America. When asked about the importance of survival, the agency's own gold standard for a trial, the official response was "they failed to meet their primary endpoint." A big help that. Their inability to hold a discussion could have had terrible consequences for thousands of patients.
But this problem is explainable - money - but the other mistake that almost derailed Provenge was inexcusable, a true "Mike Brown" moment, a near Katrina of drug evaluation.
Here is what happened - at the end of a tough eight hours, the panel votes on two issues - safety and efficacy. Here is how the questions were posed on the FDA website before the meeting and at the end of the meeting on slides.
• Does the submitted data establish that sipuleucel-T (APC-8015) is reasonably safe for the intended population?
• Does the submitted data establish the efficacy of sipuleucel-T (APC-8015) in the intended population?
The first vote went 17-0 in Provenge's favor - even the hard nosed folks more comfortable with CDER regulations and processes agreed the safety profile was very favorable, especially compared to the other possible treatment, a form of Taxotere. Then the fun began - the person chairing the session asked the second question.
I am not naming names - but imagine a serious, steady, super successful physician who knows patients are dying horrible, painful deaths with no possible treatments debating this question, out loud, with himself. "Yes, it looks like it works - but, established, I don't know..." and on and on and on and finally, after ten minutes, a no vote.
Panelist number two - same problem. They wanted to vote yes, but, well, I am a scientist, you asked if the efficacy is established the trials were small, and so on and so on and I must vote no.
Ditto for panelist number three.
At this point magic entered the room - maybe Frodo came in wearing the Ring of Power and invisibly touched the heart of the head of the committee. She asked it he panelists would like the question re-worded as they were having such difficulty with coming up with an answer they found suitable. And, let me sidetrack you again with something important.
During their testimony, Dendreon discussed a trial currently being enrolled with a target size of 500 patients, 400 already in the trial. Everyone agreed the statistical output of this trial would answer all the statisticians' questions - but the trial would not be over until the middle or end of 2010 and an application would not come up before the FDA until 2011. I did the math and that meant something like 380,000 patients might miss out on Provenge if they had to wait that long and most would die waiting. Panelists had asked if the company would provide unlimited access to the drug awaiting the trial outcome - which means providing free treatment for four years. The company hemmed and hawed, unprepared for this and finally said it was not feasible. So during the vote, this trial hung over everyone's head - it was what everyone wanted but four plus years is a long time.
Let's get back to the vote - just as the head of the committee asked if the question should be re-phrased, a slightly built, fiftyish man stood up from his seat next to the far wall, walked a few steps to her, whispered in her ear and handed her a slip of paper, and history was made. The chairman said the question posed by the FDA, was, well, not the language of FDA regs, and a new question should be posed and should read "Does the
submitted data provide sufficient evidence of efficacy.
As I wrote so eloquently in my newsletter, using the best scientific language "Ba Da Bing!"
With this new question in hand, the first three panelists reversed their votes and the countdown began. At the ninth yes vote, the media relations person for Dendreon standing next to me began to cry; the final vote was 14-3 although the FDA, true to form, recorded it as 13-4. A drug with a minuscule trial and a failed data set had garnered approval.
What next? The FDA has to formally approve the treatment no later than May 15. They could reverse the decision, they could do a lot of things. Tell me what you think, here, or read my letter as I handicap the possible outcome and cover this as news and opinion break. And please, write your Congressman and tell them to trade one Alaskan bridge to nowhere for an FDA staff that can read their own regs, speak English well enough to doe their job and maybe even run a meeting.
Comments (5)
I enjoyed your empassioned description of the play-by-play action at the Dendreon Advisory Panel hearing, Michael. I'm a recent Biotech subscriber and am looking forward to taking advantage of your experience, knowledge, and access to intelligent info in the biotech space. A few DNDN questions... 1) Do you expect the FDA will wait until 5/15 to render a decision? Or is it more likely that the decision comes sooner? 2) I was unclear as to what "an 80-90% probability that the FDA will simply say go ahead and allow the ongoing trial for Provenge to continue" means. Are you saying that it is quite likely that Dendreon can begin marketing Provenge while the new 400-500 patient trial continues? 3) The stock has settled back to $15, how likely is it that a conditional approval is given, and what do you think that news would do to the stock? 4) Are you expecting Dendreon to offer more shares as part of their shelf offering post-approval vs. pre-approval? (I'm thinking that if the company realistically expects approval it would be wise for them to announce a secondary offering post-approval, and the fact that they haven't had their offering already may indicate that they are expecting approval.) 5) Any additional Dendreon thoughts? Thanks for your excellent and timely Dendreon coverage so far, Michael. I'm looking forward to your continued updates.
Posted by Bill Poppe | April 22, 2007 10:51 PM
Posted on April 22, 2007 22:51
YOU ARE VERY BIASED AND PROBABLY SHORT THE STOCK.
Posted by jACK sIMND | April 23, 2007 2:26 AM
Posted on April 23, 2007 02:26
Michael, excellent comments as usual, I am glad that you were at the meeting. Kudos! jtorre
Posted by Joe Torre | April 28, 2007 8:39 PM
Posted on April 28, 2007 20:39
bladder cancer
Posted by bladder cancer | May 27, 2007 8:04 PM
Posted on May 27, 2007 20:04
The Unreachable Availability of Provenge
Terminal patients are those who are not expected to live due to usually illness such as advanced cancer. If the patient has 6 months or less to live, those patients are considered terminally ill. Regardless, if a patient is terminal, they are without a cure or a tolerable treatment for their illness. Since such The patients will likely die in a short period of time, treatment options, even if unproven, are often desired by such patients. This is understandable, because at such a severe stage of illness, such as prostate cancer, possible extension of their lives with comfort is worth it to them, regardless of lack of evidence of proof of whatever treatment that may be advantageous to them regarding these issues. The FDA, however, claims authority on the treatment options of such patients, although that administration has proven itself over the years to be rather inadequate with its frequent drug recalls and black box warnings, and they do these things only under pressure from the public, usually. So, the FDA may not be an ideal judge regarding such issues as treatment options for very sick patients.
Prostate cancer is rather frequent, with between 10 to 20 percent of men predicted to acquire the disease during their lifespan, resulting in about 30,000 deaths a year from this disease. It is the third most common cancer one can acquire, and the United States has the most cases diagnosed n the world, which usually strikes men past the age of fifty. One million do have prostate cancer in the United States, and about thirty thousand will die from the disease each year. Furthermore, there are different stages of prostate cancer, and the more severe the prostate cancer cases are, the higher of what are called Gleason Scores will be, and the severe cases are the most difficult to treat, of course.
Yet innovation still exists in medicine. A few years ago, a small Biotechnology company called Dendreon was working on a conceptually new treatment for the worst prostate cancer patients, and this treatment therapy created by Dendreon was named Provenge. Provenge is the first immunotherapy biologic treatment for the progressed prostate cancer patients. Usually, these patients are unresponsive to usual treatment methods for prostate cancer, and are left with chemotherapy, specifically a hazardous drug called Taxotere, as their only treatment option at such a traumatic stage of prostate cancer. Understandably, most patients at this stage refuse treatment entirely, largely due to the brutal side effects of such chemotherapy treatments as Taxodere, which include cytotoxic side effects and haematological adverse events. The immunotherapy method developed by Dendreon requires the removal of white blood cells of the diseased patient and, after altered, are re-injected into this patient now designed to attack within the diseased body what is called PAP, which is on prostate cancer cells only. This treatment requires only three such injections in a period of six weeks. This results in life extension twice that of Taxodere, and Provenge is free of the discomfort of the only other treatment of Taxotere. The medical community and survivors of prostate cancer were elated and waited with great anticipation for access to this treatment method.
Fortunately, as the years passed, Provenge, by 2007, had convinced others of its safety and efficacy in its benefit for severe prostate cancer patients. This caused great joy to such patients and their families. Perhaps greater elation was experienced by the caregivers and specialists of such a disease, such as Urologists and other caregivers who treat such patients. While Provenge was on fast track status at this time at the FDA, as they at the time agreed with the benefits of this new therapy, the FDA panel recommended with clarity the approval of Provenge based on its proven and superior efficacy and safety that was demonstrated in its trials, as they announced in March of 2007. Lifespan extension of severe prostate cancer patients was twice as long with Provenge versus Taxotere, which is the only other treatment indicated for this stage of prostate cancer that had only superficial efficacy, and is free of the toxic effects of this chemotherapy agent.
Now for the bad news: With great shock and surprise, the FDA agency rejected the approval of this great treatment for very sick patients due to, they said, 'lack of data' in May of 2007. This contradicts their favorable opinion of Provenge weeks before delivering this terrible news. Especially when one considers the FDA Commissioner is a prostate cancer survival himself! Many found this ruling completely unbelievable.
Soon after this judgment was passed by the FDA, conflicts of interest were discovered by others. For example, a member of the FDA agency who was evaluating Provenge, Dr. Scher, was found to have a financial commitment to a future competitor of Provenge that was being produced by a company called Novacea, and this company had signed a co-promotion agreement with Schering to provide support for this similar prostate cancer drug treatment being developed by this company. Dr. Scher never disclosed this conflict during the approval process of Provenge. As it turns out, this anticipated prostate cancer drug made by Novacea was discovered to have serious flaws, and Schering pulled out of the agreement with Novacea. In addition to this incident and before May of 2007, baseless letters were anonymously delivered to the FDA stating negative qualities about Provenge that were without Merit and speculative claims about the treatment were fabricated in these letters, it is believed Oncologists were speculated to lobby and pressure the FDA not to approve Provenge due to anticipated revenue loss. Yet overall, the disapproval by the FDA of Provenge angered and saddened many, and a newly formed advocacy group called Care to Live filed a lawsuit against the FDA for their clear lack of etiology for not approving Provenge, as they should have, according to the data about the therapy last year.
Terminal patients, I surmise, desire comfort during their progressive disease that has placed them in the last chapter of their lives, and certainly should have a right to choose any treatment that possibly could benefit them. Clearly, because of their lack of desirable and beneficial treatment options, most are willing to assume any risks of unapproved, yet potentially and likely beneficial treatments such as Provenge. Because they have a terminal illness, these benefits provided by Provenge take priority over any possible safety issues of unapproved treatments for them. The controversy could be concluded by a terminal patient signing a waiver of some sort, perhaps, stating that they are responsible for the consequences of an unapproved treatment regimen such as Provenge. Yet the FDA, with reckless disregard and with deliberate intent, denied what likely was a great treatment therapy for these very ill patients. Several have concluded that the FDA ultimately harmed others more by not approving Provenge, or offering any valid explanations explaining their action. Thier action was irrational, as one considers the agreement of the FDA and others regarding the need of the benefits provided by Provenge for the sickest of the sick with advanced prostate cancer.
The FDA does in fact presently have the ability to grant what is called conditional approval for such treatment methods as Provenge at this time, and why they have not remains completely unknown. What is known is that they are accelerating and worsening the illness, an illness the FDA pledged to protect so long ago. So now the FDA appears to be a bought, corrupt, and incompetent administration without loyalty and dedication to the public and its health, but with what appears to be overt collusion with venture capitalists and corporations. This needs to be corrected in any way possible for the lives of others- regardless of their own present health state today. Because of the FDA's flaws in the past regarding drugs taken off the market along with increasing black box warnings of other drugs, which happens often with both, the individual should be the deciding factor in such matters of deciding thier treatment course presently, along with their health care provider, due to this unreliable administration called the FDA.
"Facts do not cease to exist because they are ignored." --- Aldous Huxley
Dan Abshear
Posted by quiact![[TypeKey Profile Page]](http://blogs.investorplace.com/biotechblitz/nav-commenters.gif)
|
October 8, 2008 3:25 PM
Posted on October 8, 2008 15:25