November 07, 2005
Rx: The War on Cancer
I will also ask for an appropriation of an extra $100 million to launch an intensive campaign to find a cure for cancer, and I will ask later for whatever additional funds can effectively be used. The time has come in America when the same kind of concentrated effort that split the atom and took man to the moon should be turned toward conquering this dread disease. Let us make a total national commitment to achieve this goal. America has long been the wealthiest nation in the world. Now it is time we became the healthiest nation in the world.–-President Richard M. Nixon in his 1971 State of the Union address.
I. THE SITUATION AT PRESENT
The famous Greek doctor and the author of the Hippocratic oath defined cancer as a disease which spreads out to grab parts of the body like "the arms of a crab". What proves fatal for the victim is the spread of the cancer cells beyond the site of origin, and in this sense, it was a thousand years later that Avicenna of Baghdad, noticed that “a tumor grows slowly and invades and destroys neighboring tissues”. Faithful to its name in more ways than could possibly have been anticipated by Hippocrates, the disease which has launched the $200 billion “War on Cancer” in America continues to spread, invading the lives of almost every family. Based on available data, there were 10.9 million new cases of cancer worldwide, 6.7 million deaths, and 24.6 million persons who had been diagnosed with cancer in the previous five years. Like in many other areas, unfortunately the USA is leading this one as well. More than 1.5 million Americans develop cancer each year claiming some 563,700 lives, killing more Americans in 14 months than the combined toll of all wars the nation has ever fought (a new cancer is diagnosed every 30 seconds in the United States, about 1,540 dying each day from their disease). A look at the worldwide incidence of cancer raises some puzzling issues, especially related to the unexpectedly high incidence of cancers in the USA:
If we ascribe the increased incidence solely to the aging of the population, then why is the incidence so much higher in the USA than in some of the developed countries where life expectancy is comparable? On the other hand, if lifestyle is more important as suggested by the association of smoking and cancers of the lung, then why is this incidence not equally high in countries where people smoke at least as much as in the USA? One answer could be that the smokers in countries such as South America or India do not live long enough to develop cancer. However, the incidence of lung cancer in Sweden with an average life expectancy of 80.3 years is less than half of that in the USA which has a life expectancy of 77.4 years ((22 versus 55.7 per 100,000 respectively) even though 22% adults smoke in both countries. This suggests that lifestyles may be important, but that smoking may not be the only important factor.
Table 1. Approximate incidences of daily smoking among adults in different geographic areas.
Sweden |
Europe |
Eastern |
the Middle |
Turkey |
The rest of |
South |
Africa | |
Man
|
22 |
46 |
60 |
41 |
63 |
44-54 |
40 |
29 |
Female |
24 |
26 |
28 |
8 |
24 |
4-7 |
21 |
4
|
Källa: Tobacco Alert. Geneva: World Health Organization, Programme on Substance, 1996
The idea that genetic predisposition to cancer may have something to do with these high American numbers has been largely laid to rest by the experience of the Japanese who immigrated to America. Both the incidence of cancer, as well as the types of cancer, were quite different between the fresh immigrants and their American counterparts, however these differences disappeared in the second generation Japanese Americans who adopted the local lifestyle.
II. PROBLEMS IN THE FIGHT AGAINST CANCER
President Nixon declared the War on Cancer 34 years ago using the 100 words which stand as an epigraph for this essay. Acknowledging the fact that the tools necessary to accomplish the task were missing, the mandate was to invest money in research and apply the results to reduce the incidence, morbidity and mortality from cancer. After spending approximately $200 billion (if we add up the taxes, industry support etc) since 1971 on this war, 150,855 experimental studies on mice and publication of 1.56 million papers, the results can best be summarized in this one graph:
While deaths from heart disease have declined significantly in the last 30 years, the percentage of Americans dying from cancer, save for those with Hodgkin's, some leukemias, carcinomas of the thyroid and testes, and some childhood cancers, is about the same as in 1950. For the last twelve years, there is a 1% decline annually in cancer mortality. Early detection has had some significant impact, but once the cancer has spread, the outcome has generally not changed for the last half a century.
As someone who has been directly involved in cancer research since 1977, and obsessed by it for longer, I am a first hand witness to the by now familiar cycles of high expectation and deflating disappointments which have been its hallmark for the last three decades. Because the stakes are so high, both in terms of life-death issues as well as the staggering nature of the finances involved, emotions tend to run high on all sides. In this, and a series of subsequent essays, I would like to summarize some of the rather obvious reasons why this war on cancer has not manifested the anticipated, tangible signs of victory so far, as well as the dramatic gains that have been achieved at the scientific level as a result of this unprecedented investment in basic science. I hope that at the end of it all, you will be able to view the score-card dispassionately and declare a winner.
- Even though President Nixon, and subsequent administrations have continued to invest heavily in cancer research, the dedicated budget for the National Cancer Institute alone rocketing up to more than seven billion this year, the monies are not being spent as wisely as they could be. For example, the funding agencies tend to reward basic research being performed in Petri dishes and mouse models that bear little relevance for humans, 99% investigators using xenografts. Imagine the exceedingly contrived scenario of achieving a “cure” in a severely immune-compromised animal injected locally with human tumor cells and then treated with a strategy being tested. Is it a surprise when the results cannot be reproduced in humans? Basic cancer research may one day be successful at identifying the signaling pathways that determine malignant transformation, however, it will be a long time before the entire process of cancer initiation, clonal expansion, invasion, and metastases is understood, especially in the context of the highly complex, poorly understood micro-environment in which the seed-soil interaction is occurring. Using this approach, an effective therapy for cancer can only be developed essentially after we understand how life works. Can our cancer patients afford to wait that long? Isn’t the history of medicine replete with examples of cures obtained years, decades, and even centuries before the mechanism of action was fully understood for these cures? What about digitalis, aspirin, cinchona, vaccination? Another problem with the funding is that the basic scientists have encouraged each other to focus on defining the earliest molecular events even though >90% cancers kill through expansion and metastasis, 92% of the ~9,000 grants awarded last year having no mention of the word metastasis.
- There is an odd love-hate relationship that has developed between Academia and the Pharmaceutical industry. On the one hand, major research and development (R&D) efforts by industry, conducted under great secrecy, result in the identification of potentially useful novel agents which nonetheless must ultimately be tested in humans. Credible clinical trials in human subjects are conducted by academic oncologists. On the other hand, advances being made in the laboratories of academic researchers need the partnership of industry for commercial and widespread application. This forces the Industry and Academia to become reluctant bedfellows. Roughly 350 cancer drugs are in clinical trials now.
- In order for a drug to show efficacy, FDA demands that it be tested first in animal models that are not relevant to humans. To make matters worse, when the drugs are approved for human trials, they can only be tested in terminally ill patients. Many agents that would be effective in earlier stages of the disease are therefore thrown out like the baby with the bathwater. Finally, the end point sought in most drug trials even in end stage patients, continues to be a significant clinical response. Very few, if any, surrogate markers are used to gauge the biologic effects of the drugs. The surrogate or bio-markers include proteins being produced by the abnormal genes, as well as processes and pathways that distinguish cancer cells from normal cells such as formation of new blood vessels or angiogenesis. If a drug does not produce the desired clinical end point, it is then likely to be abandoned completely, even though its biologic activity could be harnessed for more effective use in combination with other agents.
- As the internet dotcom bubble burst in the 90s, the bi-technology industry was the big winner since some of the best minds in the country made lateral moves and began to invest their talents in this area. The striking change over the last decade in the pharmaceutical industry has been its ability to attract and retain high caliber academic scientists and clinical investigators. Even with this vital infusion, it takes 12-14 years and a prohibitive ~800 million dollars for a pharmaceutical company to get a new drug approved, most of the money having been raised from the private sector which is clamoring for a profit. Following the arduous R&D process and the tedious, time consuming and labor intensive animal studies, by the time a clinical trial is undertaken in human subjects, the stakes are already too high and companies may have to be struggling to demonstrate the tiniest statistical benefits over each other’s products.
- The catch phrase today is “Trageted Therapies”; the concept that a convergence of science and advanced technologies will illuminate the cumulative molecular mechanisms that ultimately produce cancer, and this will lead to an objective drug design to pre-empt or reverse the cancer process. Except for the drug Gleevec developed against Chronic Myeloid Leukemia (CML), a rare type of leukemia in which single gene mutation underlies the pathology, all other Targeted therapies so far have met with modest successes. For example, the recently approved Erbitux and Avastin for cancer of the colon and rectum improved survival by 4.7 months when given in conjunction with chemotherapy. Even in the area of targeted therapies, the efforts are frequently scattered. Academia, Industry and Institutions such as the NCI, FDA, CDC, EPA, DOD etc are not coordinating their resources efficiently. For example, hundreds of researchers across the nation are performing gene expression and proteomic experiments, diluting the number of specific cancers examined for potential targets instead of developing organized collaborative studies.
- Research on such topics as epidemiology, chemo-prevention, diet, obesity, life-styles, environment, and nutrition is woefully under-funded.
III. WHAT SHOULD BE DONE TO FIGHT THE WAR MORE EFFECTIVELY
"Stomach cancer has disappeared for reasons nobody knows and lung cancer has rocketed upward for reasons everyone knows," says John Cairns, a microbiologist now retired from the Harvard School of Public Health. To win this war, some steps that need to be taken are rather apparent while others remain to be carefully debated and planned. For the vast majority of cases, no “cause” can be identified, but cancer is presently believed to be triggered by a combination of genetic predisposition and lifestyle factors such as diet and occupation. Consequently, chances of developing cancer can be significantly reduced by not smoking, adopting a healthier lifestyle, and proper nutrition. Focus is needed in improving methods for early detection, on treating precancerous conditions, (the dysplasias, metaplasias), and on understanding the reasons for susceptibility to the malignant process in individuals and families.
Where research is concerned, man must remain the measure of all things. Human tumors rather than mouse models should be studied directly. To harness rapidly evolving fields like nanotechnology, proteomics, immunology, and bioinformatics, and focus them on serving the cause of the cancer patient, we must insist on collaboration between government institutions (NCI, FDA, CDC, DOD etc), academia and industry. In the case of the Human Genome Project, collaboration was the key to the rapid mapping. The same concerted effort needs to be invested now in sequencing mutations in hundreds of freshly obtained human cancers of all types, a venture which has been proposed as the Cancer Genome Project. It is a well known fact that all those machines and robotics developed worldwide for sequencing the human genome are either sitting idle or being used for sequencing the genomes of microorganisms and fruit flies. They would serve a far better purpose by being employed in sequencing several hundred breast, lung, colon and prostate cancers to identify the most common mutations. Identification of specific mutations will lead to the discovery of seminal signaling pathways unique to organ specific malignant cells which can then serve as therapeutic targets. Given that nature is highly parsimonious, it is likely that some of these pathways would be redundant as was the case with Gleevec. This drug was developed specifically to inhibit the tyrosine kinase of the Abl gene, and has proved to be effective in producing remissions in >97% CML patients. However, it has now been discovered that patients with gastro-intestinal stromal tumors or GIST can also respond to this drug as the cells use the same tyrosine kinase blocked by Gleevec. More recently, thyroid papillary cancers, subsets of patients with other bone marrow disorders (for example those showing translocations between chromosomes 5 and 12) and even cases of as different a disease as pulmonary hypertension, have been found to respond to Gleevec. What this proves is that some key pathways are likely to be present in cancers or even diseases across organs, and their identification could deliver unexpected benefits.
Cancer is a multi-step process that involves initiation, expansion, invasion, angiogenesis and metastasis. Each stage of the disease may offer a variegated set of targets, thereby making the one drug, “magic bullet” approach only feasible in a handful of cancers where single mutations underlie the malignant process (as described above for CML and Gleevec). A critical lesson from developing successful therapy for AIDS is that three drugs targeting the same virus had to be used before effective control of its replication was achieved. Similarly, multiple targets must be attacked at the same time in the cancer cell. The “seed and soil” approach where drugs act on both the malignant cells and their microenvironment would be preferred over those targeting either in isolation. For example, a drug that blocks a key deregulated intracellular signaling pathway and checks the malignant cell’s perpetual proliferation can be combined with an anti-angiogenic drug which stops the formation of new blood vessels and arrests the invasion of tissues by the tumor. The objective choice of agents would require the practice of evidence-based medicine, and this is what the government institutions should be rewarding the investigators for. Many effective therapies directed against components of the seed and soil, are already available, but researchers are only allowed to use one investigational agent at a time, and that too in patients with advanced disease. This stilted and almost self-defeating approach needs to be abandoned. Patients who already have a diagnosis of cancer cannot afford to wait.
I am optimistic that in the next few years, given the power and sheer velocity of the evolving bio-technology, the very fundamentals of cancer research and treatment will have undergone cataclysmic changes. It may not be possible to cure cancer within the next decade, but, in the words of the NCI Director, Dr. Andrew von Eschenbach, it may very well be possible to “transform cancer into chronic, manageable diseases that patients live with - not die from”.
Posted by Azra Raza at 12:05 AM | Permalink
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Comments
Brilliant summary, Aps! I learned much from your essay, which is a much-needed accessible introduction to what has been going on in cancer research for decades, and even more importantly, what should be happening now. I really look forward to future installments with more details. Keep 'em comin'...
Posted by: Abbas Raza | Nov 7, 2005 12:57:53 AM
In the book "Otto Warburg Cell Physiologist, Biochemist and Eccentric" by Hans Krebs and Roswitha Schmid, Clarendon Press, Oxford, 1981, the following statement is made on pages 7 and 8.
"In 1913, at the age of 30, Warburg was appointed 'Member' of the Kaiser Wilhelm Gesellschaft(4) to take effect 1 April, 1914. This was an appointment as head of a research department, which gave him complete freedom in the choice of his research subject and involved no teaching or administrative responsibilities whatsoever. The main movers in bringing about this appointment were Theodor Boveri, the biologist, and his former teacher, Emil Fischer. Fischer described the attitude of the Kaiser Wilhelm Gesellschaft as follows when in 1911 he (successfully) persuaded Richard Willstatter to accept a similar post:
'You will be completely indepedent. No one will ever trouble you. No one will interfere. You may walk in the woods for a few years or, if you like, may ponder over something beautiful.(73)'
On the whole, this policy (which rested on extreme care and competence in selecting the right people) paid magnificent dividends: Warburg, Einstein, Haber, Hahn, Meitner, Correns, Goodschmidt, Polanyi, and many others were 'Members' who made the fullest use of the opportunities..."
These passages are quoted because they illuatrate a procedure for producing great and original and new scientific discoveries in the past in Germany. Obviously, while the United States' scientists win most of the Nobel prizes, something is obviously very wrong in the arena of cancer discovery and research. Yet, every year our elected "leaders" simply return to business as usual and continue to pour money down the same old failed pathway, of not only failed research areas some of which are touched on above, but with little said about the obstruction to new ideas and downright fraud of the medical orthodoxy, as documented in books like "The Cancer Industry" by Ralph W. Moss, Ph.D., 1996, first published as early as about 1980.
Conflicts of interest are likely the single most prominent issue preventing new ideas from being investigated and demonstrated. But government burearacracies do not like to change directions, let alone admit mistakes. And fortunately, for them, a gullible and unwitting public is complete disorganized in knowledge and willpower, to compel any meaningful change in direction. And so business as usual it will be, continuing to reward failure, with organizations like the American Cancer Society, with the help of the cowardly media, acting as a cynical cheerleader, to divert attention from the continuing failure of the false war on cancer, with one person dying about every minute in the U.S., either of cancer or treatment or a combination thereof; but fortunately for the medical orthodoxy, no one every knows for sure, because routine autopsies of cancer victims, by a thoroughly independent and excellent laboratory, as a condition for receiving treatment, are not required; hence the blind continue to follow the blind.
A great deal is already known about cancer, but one would not know this talking to most medical doctors or reading the pronouncements of the medical orthodoxy.
A new broom sweeps clean. Most of the "cancer generals", who must bear the responsibility for the loss of the many "battles" of this war, must be fired, dismissed, and replaced with others, carefully chosen as described in the quotation above, and given complete freedom and independence. Only then, can we have an iota of a chance to solve this problem, first from prevention, then, failing that, from treatment.
Posted by: Winfield J. Abbe | Nov 7, 2005 7:24:48 PM
Dear Az:
An excellent essay on the global problems facing research on cancer therapy and reasons for it's failure so far, inspite of infusion of immense amount of money into it. This has put a lot of things into perspective for me. The only surprise was that after criticizing the NIH and other Governement agencies for the way they reward research dollars you ended the article by quoting the director of NIH for likely sucess in the future. If he understands the issues the way you describe then why is he not changing the way NIH disburses the research money accordingly? Enjoyed the piece very much and look forward to your future essays.
Posted by: Tasnim | Nov 8, 2005 9:25:00 PM
Great essay, Az! Very informative.
Posted by: Bibi | Nov 8, 2005 10:29:47 PM
This essay makes some important, excellent points. An additional challenge to developing successful new cancer therapies is the level of bureaucracy that has become attached to clinical studies in the contemporary era. Once all the various internal and external institutionall committees, statisticians, administrators, lawyers, institutional review boards, and other interested parties have reviewed a proposed study and finished arguing about it, years may have passed... and many additional patients passed away during them. Big academic centers and cooperative groups dedicated to cancer treatment are particularly plagued by this problem. This rarely accomplishes the goal of protecting the patient - instead, it just stymies creative work and makes drug development (and subsequent pricing) much more expensive.
Posted by: David Steensma | Nov 9, 2005 8:21:52 AM
Very insightful for a lay person like myself. I look forward to reading future articles as you share your ideas with the relevant communities that can make a difference, modify approach and stem wastage of resources.
Posted by: Mariam | Nov 9, 2005 8:32:15 AM
This is a thoughtful and elegant summary of the state of cancer research. The Federal Government deserves credit for providing several avenues of funding, with the bulk of the resources appropriately committed to basic research. However, overreliance on the NIH as a source of funds has, in turn, produced several frustrations:
1. Hypothesis-testing, the central dogma of NIH grant models, seems to be the only way towards funding, stifling other avenues of cancer research.
2. The wholesale skewing of NCI grants towards animal models of little relevance. This is self-perpetuating as successful grantees sit on the study sections.
3. Bureaucratic inertia under the guise of "patient safety" delays clinical trials as highlighted by Dr. Steensma.
The essay also offers guidance towards the future.
It debunks the popular preoccupation with targeted therapy and the quest for a "magic bullet" like imatinib (Gleevec. The success with imatinib, unfortunately hyped by the media, is unlikely to ever be replicated outside of CML because most human cancers have redundant pathways [Hahn & Weinberg Nature Rev. Cancer 2, 331−341 (2002). Rangarajan & Weinberg Nature Rev. Cancer 3, 952−959 (2003).] Instead, a thorough understanding of systems biology in is most likely to reveal the essential non-redundant pathways that need to be targeted simultaneously.
We also need to focus on early stages of carcinogenesis. Clinical trials at the terminal end of the cancer spectrum are often futile, as advanced disease is least susceptible.
Mandating a limited autopsy as a condition for participating in clinical trials is a great suggestion. This may sound cynical but I expect that the very bureaucratic machinery that is supposed to help with the development of clinical trials will find some strong objections to frustrate this proposal.
While I construct my wish list, another issue is one of visionary and inspiring leadership from the NIH. To have credibility, the appointment of the NIH director and the directors of individual institutes must be made exclusively on the basis of merit.
Posted by: Minoo Battiwalla | Nov 9, 2005 10:36:38 AM
A very timely and thought-provoking essay. I consider myself to be a practical (as opposed to a theoretical)person, not that I consider one is better than the other but I recognize that perspectives from both are needed to create a balanced argument. The suggestions presented in the para on stomach cancers and lung cancers etc are the ones which I believe are the most criticalones for immediate adoption and application and yet these are also the hardest to achieve. Cessation of smoking and other tobacco-habits will guarantee a substantial reduction in the incidence of cancers of the lungs and of mouth and head and neck, all taking a disproportionally high toll among all cancers. Likewise, making Pap-smear universally available and mandatory (as is the case in all "developed" countries )in the "under-developed" world will also result in a major reduction in the mortality and morbidity that have been taken for granted among the latter group and the numbers of women who suffer from that completely preventable torture is shockingly high.
But achieving the above-noted goals are so very difficult that one tends to almost give-up before even starting. These preventable cancers are so intertwined with poverty and lack of education and all other ills which are the scourges of the poorer nations that unless those "primary" maladies are attacked first and the socio-economic and educational standards are improved there, Pap-smears and ridding the society off tobacco use will continue to remain words in essays and verbal arguments without making impact on the underlying problems.
I take issue with attack on "targeted therapies" and want to point out that emergence of Gleevec, although, by no means a panacea, did result in a high level of renewed excitement and interest and enthusiasm among scientists and doctors and thus made the public at large to look again at the overall increased respect for cancer research and cancer researchers. That is a boost in morale which should not be overlooked.
I thank Azra for writing such a beautiful essay and inviting us to write a commentary. That is what we all love in Azra, an open-minded human being.
Posted by: Kanti R Rai | Nov 9, 2005 12:45:49 PM
Very interesting and informative article. However cancer is a very complicated game and issues cant be explained in a simlplistic way. I share Azras frustation at the slow pace of achievements in cancer treatmen, however the view from India which houses every seventh human being on this earth are more mundane. The country has not yet been able to deliver on basics like clean drinking and safe water to its masses. Millions are still dying of malaria, cholera, typhoid, malnutrition and lately of AIDS. Even in the field of cancer India has failed to enforce tobacco control, 30- 40% cancers in India are tobacco related and hence preventable. There is no mass screeing for breast cancer, there is no mass screeeing for early dectection of cervical cancer. We in India feel that people in the Western world have crossed these hurdles long ago, their thresolds and expectations are higher. Countries like India save more lives by community programmes like cessation of smoking, mproved hygiene for cervical cancer and reduction of pollution. India has a lot of catching up. Major advances in cancer treatment can have only a limited imnpct on the cancer scene in India, as mass delivery of these methods are prohibitively expensvie. As Nehru said we have miles to go before we can catch up with the western world.
Posted by: Vinod Raina | Nov 10, 2005 12:01:26 AM
A wonderful easily understandable golobal perspective. I really enjoyed reading the article. As you said, all approaches have advantages and limitations and the balance needs to be wieghed carefully and kept in mind for allocaion of funding. The balance between funding for basic research and clinical research and translational research has to evolve in a rational manner. The major problem with research funding in the West is the extremly high administrative overheads in both industry and academia and thus when the final product comes in the market it is beyond the pocket of the common man even in the West let alone in the developing countries. There is an urgent need for the developing countries to have a buy in the process which can offset some of the cost. One way would be outsourcing some of the research in countries with less administrative overheads without compromising the quality of research. This has been done for other industries so why not research.
I hope you will address some of these issues in your future articles
Posted by: Rabia Hussain | Nov 10, 2005 7:53:29 AM
I did not find that the essay ascribes conflict of individual interests within the whole of bureacracy as a solitary barrier but one of those unfortunate growths from a bureaucratic web. That is one of the greatest strengths of the essay for an in-depth analysis into the history and present state of affairs within the "War on Cancer." The economic nature of decision making in bureaucracy may be too intricate to cover in a single essay, and thus I would find it unapproachable to add more in this field. In fact, I find that the fundamental source of the situation is remarkably expressed here. And challenging that at a socioeconomic level of public health would step too far into the role of a sociologist, where the root of the problem is just what the essay fundamentally asks: what can be done following the most plausible hypotheses of the day and manipulating ever-growing variables within lasting theory. A similar confusion in practical testing of hypotheses occurred in the more theoretical field of evolutionary biology some forty years ago. And since then, the strides and collective pace of those strides has been remarkable.
Dr. Raza has produced a most fascinating essay at multiple levels, to be read across strata of knowledge on the subject. Just where secondary issues should be dealt, they are, but then linked to the whole, which has been a fundamental to my understanding of any concept in text, foreign or well drawn in my vocabulary. Teach and continue. It is an essay worth sharing, indeed a brilliant display.
Posted by: James Crowley | Nov 10, 2005 9:38:16 PM
Dr. Raza's essay certainly points to a number of issues which impair cancer research and the eventual development of significant improvements in cancer care. There are three issues that need underscoring.
1. Enormous progress was made during the 70's, when it was possible for an investigator, with little paperwork and approvals, etc, to launch an investigation following his own hunches. We would have never developed curative therapy with cisplatin combinations in testicular cancer under the current system. First, no one would have selected testicular cancer as a rational target -- too rare. Second, cisplatin was very toxic -- the company would have quit supporting development of the drug early fearing litigation. Third, original studies with the agent in the more common tumors were very dissappointing. It was because several investigators rapidly built on previous investigations that curative therapy was achieved in about three years following initial human trials. Now it takes nearly a year to be allowed to test a new agent in a new tumor (given IRB approvals, funding, etc)
2. The FDA needs to modernize its one size fits all system. Approval for a new antibiotic should follow very different rules than approval for a new cancer drug. It should not cost 800 million for a drug company to develop and bring to market an effective agent. Cancer patients who have run out of standard options are usually eager to be "guinea pigs" for new agents, and instead of confining phase I - II studies to the major centers (in itself a highly political decision) these agents should be available with little paperwork and at the community level. Systems to protect patients can be developed which are far more streamlined and useful than the current system. Any street corner oncologist could probably devise a better system than we have.
3. We know much of cancer is life-style related. Tobacco products contribute to 30 to 50% of all cancers in the United States. We could do more to battle cancer than anything else by simply taxing the hell out of tobacco products, and using the tax for something useful. If people had to choose between eating and smoking, you can be certain the rate of cancer would decrease. Unfortunately, our political leaders are severely dysfunctional, and I doubt we will see positive changes in our lifetimes.
Posted by: Don Higby | Nov 14, 2005 2:48:28 PM
This is a very informative essay. I truly admire your zeal and passion for fighting cancer. It was also fascinating to learn about the economics of cancer treatment. As a fellow in training, I feel extremely fortunate to be in this revolutionary times of targeted therapy. The 'seed and soil' theory is a very logical and important approach - attack at all different levels.
From a personal experience, My mother has been on Gleevac for Metastatic GIST for 3 years and she is NED. It is remarkable for a disease which had very limited treatment options prior to the Gleevac era. Gleevac surely been my life saviour and I believe that mankind will win this 'war' one day.
Thank You for your insightful article and look forward to more.
Posted by: Rasmia Khalid | Nov 18, 2005 11:56:15 AM
Comparing cancer to heart disease is not a fair comparison. The “war on heart disease” has been more successful to date than the war on cancer because of the nature of the two diseases. Heart attacks and stroke, by and large, are caused by individual factors, superimposed on a genetic constitution with variable risk. The decline in mortality of heart disease has been due primarily to recognizing and controlling these factors. Cancer, on the other hand, is overwhelmingly caused by external factors that an individual cannot control. As Azra’s chart shows, living in an industrialized society is the single most important risk factor for cancer.
Most cases of cardiovascular disease can be prevented or delayed by active participation of the individual. We now have simple screens to identify those at high risk, like heart scans and cholesterol levels. These risks can be dramatically lowered by changes in diet, increase in exercise, and – most important to Americans – pills. These pills include antihypertensives, cholesterol-lowering drugs, and aspirins. Most Americans would rather take a pill than change their lifestyle, and the pharmaceutical industry has obliged.
Compare this to cancer. With the exception of smoking cessation (and it is a very big exception!) there is very little that an individual can to do to prevent cancer. There are no dietary manipulations or exercise regimens that help very much; even sunscreen has only a small effect. Medicines which prevent cancer have serious side effects, or increase one type of cancer while preventing another. And we know almost nothing about how best to use them in high-risk patients, if we could identify who is at risk. And man screening tests which find early, curable cancers are still very invasive, and thus not widely used.
So we need to focus research efforts on these three areas – identification of genetic risk, cancer-prevention drugs, and cancer screening tests. But even if we optimized prevention and detection strategies, and stopped all cigarette smoking, we still would not be where we are with cardiovascular disease. We still have our background environment, and there will be a lot of cancers to treat.
So how are we doing on cancer treatment? Again, let’s compare to heart disease. The cure of established, advanced heart disease, especially in the elderly, is still not very good; we are probably doing better for many cancers. What is different, though, is that the approach to heart disease has changed. Cardiovascular disease is no longer an acute illness. It is treated as a chronic, lifelong condition that is managed with drugs and intervention such as bypass, pacemakers, and angioplasty, with a significant improvement in lifespan and life quality. We should be looking at cancer this way also. We should be developing treatments that allow cancer patients to live longer and more comfortably with cancer, even if cure is not possible.
I agree with Azra on her ideas of cancer research. It needs to be focused on patients, and should be more closely integrated into routine clinical practice. FDA drug approval can also be done more effectively. As pointed out, industry and academics need to work together. How can we incentivise this? Remember that the pharmaceutical industry is driven by profits. In the cancer arena, the industry is seeking extremely lucrative cancer treatment drugs, while in cardiovascular disease the lucrative drugs are those used for prevention (antilipid drugs, anti- hypertensives, etc.). Maybe this will change as the profits to be made on cancer chemotherapy begin to decline because of national price controls and pressure from Medicare.
The last point that I would like to raise is how to use national cancer research funds. Many people do not realize that easily half of the research funds from the National Institutes of Health (NIH) do not go to research, because a large share is skimmed off as “overhead” to support the universities which house the research labs. This system of grant overhead, which was legitimately established decades ago to provide research infrastructure, has become a major source of operating revenue for institutions of higher education. It has gotten to the point that faculty cannot obtain tenure, keep their salaries, or even hold their jobs, if they do not win research grants from the NIH, because the university is depending on their grants as revenue sources. Research grants become an end in themselves, rather than a means to an end (curing cancer). It would make more sense to me if funds for cancer research were used for cancer research, and other mechanisms were found for the government to support higher education.
Posted by: Carol A Westbrook | Nov 18, 2005 6:32:47 PM
Dear Azra,
I put off reading your essay for a long time because of my own battle with daily life as a primary-care physician and mother of two pre-teens.( This is also the excuse I use when I think that a particular scientific essay might be too "scientific/boring/impractical" for me to comprehend!) I'm delighted to report that I thoroughly enjoyed reading about the "real" war on cancer behind the scenes! Thank-you for making your explanations so clear.I suspect that many scientists use ambiguos vocabulary, and boring details, just to prevent average people like me from participating in any scientific debate! After reading your essay, I'm prepared to take on the politicians,industrialists and scientists on this issue......well, up to a certian point! Please continue to write more on this subject. By sparking the interest of a tired, working mother in this important issue, you have already performed a miracle!
Posted by: Waseema Sheikh,MD,MPH. | Nov 18, 2005 11:00:20 PM
Dr. Raza, I have read your article few times so far. It is powerful, informative, and enlightining. It is amazing in a time of profound advancement in cancer research, that bureaucracy and a complicated web of "political" agencies take precedent to the true focus of oncology, the PATIENT...
I thank you for recommending this article to me and I will continue being honored of having you as one of our mentors in our institution.
Amr
Posted by: Amr Hassan | Nov 19, 2005 7:27:19 PM
As a medical resident seeing pts. with different illnesses all day, I must admit there is nothing more moving than having a pt. being diagnosed with cancer. The absolute feeling of helplessness and defeat while making a cancer pt. "comfort care" is somethng which, I guess, as doctors all of us go thur much more often than we would like to.
I find your phrasing of the article apt and proper for something like cancer. It is definitely a war (or atleast it feels like that) and one which we have been sadly loosing uptill now. Found your article very informative. Your comparison on the incidence of cancer between the east and west is most striking and I would love to see another article from you regarding the resons for it. I do feel that just saying it is ill- documentation of cancers in the east is just not enough. Thankyou again for a nice article. Looking forward to the next one!!
Posted by: Fahd Quddus | Dec 1, 2005 2:45:42 PM
To win the “War on Cancer” we must address the fundamental problem, tumor cell evolution. Cancer is an enormously diverse, unpredictable, stochastic, process that results from rapid cellular evolution inside the body. The logical implications of the stochastic nature of tumor cell evolution have received insufficient consideration.
I would like to call readers attention to an editorial titled, Evolution and the Treatment of Cancer, posted by the Van Adel Research Institute:
http://www.vai.org/upload/departments/tumormetastasis/editorial01.pdf
The editorial examines requirements for the specific destruction of an evolutionary population of malignant cells, and proposes a major non-profit initiative to develop a set of drugs that satisfies these requirements – the Cure Cancer Project.
Signers on the editorial include: Dr. Emil Frei, III, Dr. Lawrence A. Loeb, Dr. Arthur C. Upton, Dr. Craig Webb, Dr. Harvey I. Pass, Dr. Michael Liebman, Dr. Richard I. Somiari, Dr. Henry Heng, and Dr. Bernie Crespi.
Thank you for the opportunity to share this with you. Arnold Glazier M.D.
Posted by: Arnold Glazier, MD | Aug 5, 2006 12:44:55 PM
The needed change in the "war on cancer" will not be on the types of drugs being developed, but on the understanding of the drugs we have. The system is overloaded with drugs and underloaded with the wisdom and expertise for using them.
Cancer patients usually undergo four or five courses of chemotherapy before medical oncologists can tell whether the treatment is having an effect. By that time, the tumor may have grown so large that it is too late to switch to another chemotherapy regimen or the patient may be so weakened by the treatment that trying another approach is not immediately feasible. Medical oncologists treat a lot of patients but they don't know going into treatment if it's going to work.
A major obstacle in controlling cancer growth and metastasis in patients is the widespread inappropriate use of anti-cancer drugs. As the increasing numbers and types of anti-cancer drugs are developed, oncologists become more and more likely to misuse them in their practice. Between 2002 and 2004, 395 cancer drugs were submitted for clinical trials.
It would be highly desirable to know what drugs are effective against particualr cancer cells before these cytotoxic agents are systemically administered into the body. Cell culture assays are tests on living specimens of cancer cells to determine the optimal combination of chemotherapy drugs. These assays are specifically tailored for each individual patient, with no economic ties to outside healthcare organizations, and recommendations are made without financial or scientific prejudice.
Recommendations are designed scientifically for each individual patient. Various assays are performed on a tumor sample to measure drug activity (sensitivity and resistance). This will determine not only what drug or combinations of drugs will not effectively work, but which will be most effective for an "individual's cancer. Then a treatment recommendation is developed through what is know as "assay-directed" therapy.
At one time, chemosensitivity testing was considered unreliable because it was only fifty percent accurate and it took too long to get the results. Today, preliminary results are completed in about seven days and chemosensitivity testing has progressed to the point where it is <90% effective.
The key to improving drug sensitivity tests is related to the number and types of drugs tested. The more anti-cancer drug types there are in the selective arsenal, the more likely the system is to prove beneficial. In order to acquire sufficient data, tumors are tested with at least two assay endpoints, and most often three, for sensitivity in any one patient. On average, up to twenty drugs and combinations at two concentrations in three different assay systems, is an effective way to avoid false-positive or false-negative data. Careful choice of drug doses and administration intervals also improves outcomes.
Conventionally, chemotherapy is prescribed by medical oncologists according to fixed schedules. These schedules are standardized drug regimens that correspond to specific cancer by type or diagnosis. These schedules, developed over many years of clinical trials, assign patients to the drugs for which they have the greatest statistical probability of response.
However, patients with cancers that exhibit drug resistance are on the wrong side of the probability curve. They will likely receive treatments that are wrong for them. A failed attempt at chemotherapy is detrimental to the physical and emotional well-being of patients, financially burdensome, and may preclude further effective therapies.
Every cancer patient should have his/her own unique chemotherapy trial based on consultation of pathogenic profiles and drug sensitivity testing data. Research and application of drug sensitivity assays are being encouraged by growing patient demands, scientific advances and medical ethics. Drug sensitivity tests are not a luxury but an absolute necessity, and a powerful strategy that cannot be overlooked.
A chemo-induced gene mutation can happen when the original chemo received does not work. The cancer comes back. When it does this, the cancer comes back more aggressively. The mutagenic effects (changes in form) of chemotherapy on a genetically-unstable tumor, drives the tumor into a state of more aggressive behavior.
A cell culture assay uses living tumor cells to determine which drug or drug combination induces apoptosis (cell death) in the laboratory. Each patient is highly individualized with regard to sensitivity to chemotherapy drugs. A patient's responsiveness to chemotherapy has its own unique individuality.
There has been a veritable deluge of new approvals of cytotoxic drugs in recent years as the tortuous FDA process has been speeded and liberalized. In many cases, a new drug has been approved on the basis of a single very very narrow indication. But these drugs may have many useful applications, and it may take years to find out. Cell culture assay testing offers a way of seeing if any of these new drugs might apply to an individual's specific cancer.
Posted by: Gregory D. Pawelski | Jan 16, 2007 8:10:52 PM
One of the greatest barriers to development is the lack of communication between different fields of knowledge.
I am not surprised that the USA has the highest cancer rate in the world. The USA has the most contaminated soil, water and air (pesticides and burning of fuels) in the world. Americans have the worst possible diet (mostly junk food). Americans are probably more exposed to vaccines and pharmaceutical drugs than any other population which may be associated with an immature and ineffective immune system unable to fight cancer cells. So really, when you look at all these factors, cancer comes as no surprise. There is only so much abuse that a body can take. Best regards, Liz
Posted by: Liz | Feb 11, 2009 12:35:51 PM
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