Lung Cancer / Mesothelioma
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Loading ...While progress in small cell lung cancer (SCLC) has been slow, over the past few years there have been leads in management of extensive disease that have introduced a potential change in the standard of care based on better results. Extensive disease SCLC, or ED-SCLC, is defined by having cancer that has spread outside of the region that can safely be covered by a radiation port (more details and relevant figure in SCLC 101 post), and this accounts for approximately two thirds of SCLC cases. Patients can often show very rapid cancer progression and clinical deterioration, but fortunately initial treatment very often leads to rapid and dramatic improvement, although we are not able to cure ED-SCLC.
Now, a history lesson. First, oncologists established that chemo combinations did better than just starting with single drugs. What emerged as the old standard chemo regimen was a combination called CAV (cyclophosphamide, adriamycin, and vincristine — can you see why we use acronyms?). Then, about 15 years ago, the relatively new combination of cisplatin and etoposide (now far from new) was shown to either do as well or better than CAV in multiple trials, and oncologists either gave alternating CAV and platinum/etoposide (or PE, as it is abbreviated), or PE alone. About 50-70% of patients had a significant reponse (shrinkage of the cancer volume by more than half), and about 10% had a complete response, with no evidence of disease after usually 6 cycles of treatment. We now have seen that in many lung cancer settings, 4 cycles works as well as more, but historically we have gone up to 6 cycles. Unfortunately, even after a good or great response, the cancer almost always returns, and it is often much less responsive to treatment the second time around, or later. “Maintenance” therapy with longer-term chemo after the first 4-6 cycles has led to a somewhat longer time before the cancer returns, but it has not yet led to any improvement in how long patients live, which is the biggest goal for most patients and oncologists.
More than a decade later, platinum and etoposide is still arguably the best way to treat ED-SCLC. Carboplatin, a newer chemo agent related to cisplatin but with less risk of kidney damage, nausea/vomiting, nerve damage (peripheral neuropathy), and hearing damage (ototoxicity), is often substituted for cisplatin now. There has been one study that compared cisplatin/etoposide to carboplatin/etoposide and found no real differences in outcomes, so many oncologists recommend carboplatin instead because of the toxicity benefit (it’s possible that it’s slightly less effective, but in the setting of disease that can’t be cured, significant differences in toxicity/quality of life can be important).
And then an important trial came out of Japan, in which 154 patients with ED-SCLC were randomized to receive cisplatin/etoposide or cisplatin/irinotecan (also known as CPT-11, or camptosar). This trial , subsequently published in the New England Journal of Medicine (NEJM) (Noda abstract here) stopped after an early look at the data, because the group that received cisplatin/irinotecan were doing so much better than the cisplatin/etoposide arm that it was considered unethical to give cisplatin/etoposide in Japan after that. The curves are shown here, and you can see clear differences between the two arms that show better survival with the newer combination:
(click to enlarge)
The toxicity profiles were different between the two arms, with more issues of low blood counts in the platinum/etoposide arm, and more diarrhea with platinum/irinotecan (diarrhea is consistently the leading major problem with irinotecan), but neither arm was clearly more toxic. So this trial led to cisplatin and irinotecan becoming the standard of care for patients with ED-SCLC in Japan.
So is cisplatin and irinotecan the new standard of care in the US? It’s certainly a reasonable option. Studies that get published in the NEJM are meant to reach a broad audience and potentially change standard practice. And in the US and otherwise outside of Japan this became a strong consideration, but it hasn’t yet been adopted as the clear best choice for first-line treatment in ED-SCLC. This isn’t because the data from Japan aren’t high quality (this is a very good oncology group that performed a well-conducted trial), but a recognition that this was still a trial with just over 150 patients, and more importantly that results in Japan can be different from results in the US or other places. First, the oncologists in Japan had more experience with irinotecan than US oncologists, as the drug was developed there. We tend to do better with drugs that we have good experience with, such as by recognizing and managing side effects more effectively. But the second and likely more important point is that irinotecan may behave differently in the more genetically homogeneous Japanese population than in a more diverse and largely European-descended US population. In fact, the toxicities of irinotecan are very significantly affected by the metabolism of irinotecan in the liver, and the proportion of people with a genetic profile predicting for toxicity problems from these liver enzymes is likely to be very low in a Japanese population but considerably higher in other populations. So it is probably worth confirming the Japanese results in other parts of the world.
Two major clinical trials were launched, and we only have the results from one of these. An industry-sponsored trial by the makers of irinotecan (then Pharmacia, now Pfizer) did a US-based trial of cisplatin/etoposide vs. cisplatin/irinotecan with a different schedule (lower dose cisplatin for two weeks out of three, with a lower dose of irinotecan on the same two of three week schedule), and this showed no benefit for cisplatin/irinotecan. The results (abstract by Hanna and colleagues here) were pretty much the same between the two approaches, so it’s not as if the irinotecan was a bad choice, but it didn’t look clearly superior to our old standard. But we don’t know if that is because cisplatin/irinotecan is really no better, or whether tinkering with the dose and schedule is the reason there was no difference.
The second trial is being run by the Southwest Oncology Group (SWOG) and is essentially an exact version of the Noda Japanese trial on a larger scale, with over 600 patients. We don’t have any results from that trial (known as SWOG 0124) yet, but we should be getting information on it within the next year or two. If this trial is positive and shows a survival benefit for cisplatin/irinotecan, it will almost certainly establish this combination as the new standard of care in the US as well as Japan, and we will no longer debate whether we have made any real progress in SCLC in the last 10-15 years.
Posted in: Chemotherapy, Core Concepts, Extensive Disease Small Cell Lung Cancer (ED-SCLC), Lung Cancer, SCLC, Extensive Disease and Recurrent, Small Cell Lung Cancer (SCLC), Treatment
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Dr West,
Thank you for this excellent article on small cell, extensive stage. I lost my husband last year to ED-SCLC and I never found a good explanation behind the recommendations for PE vs. CPT-11. Makes much more sense now and helps alleviate the ‘did we do the right thing’ nagging thoughts. Again, thank you so much.
Lynne
lynneh
Thank you, Dr. West for the continuation of these very informative posts on SCLC - I’m learning much more from you than I have up to this point from either text books or websites. Also - I happen to be a nurse so I probably would have been able to decipher some of the more challenging medical terms more readily than a lay person - but was so glad to see that you are keeping your posts readable for every person thirsting for knowledge on this disease.
I look forward to reading more.
Thanks again,
Leanne Fitzgerald
Leanne
Thanks for the information Dr. West. I am trying to get a better idea of the survival rates and have seen everything from 2 months to 10 years yet every one says it isn’t curable but people do go into remission. Can you give me an idea of what a realistic best case scenario is for someone with ED-SCLC? What are we hoping for?
Thanks,
Forsyth
I don’t want to bludgeon you with discouraging numbers, but the very impressive Japanese trial had a 2-year survival of just under 20%, and about half of the patients had died a year after starting treatment. Those are a bit better than typical US results, but they can give an idea of realistic numbers.
Dr. West, thank you for the article. It was the first time I really read a solid explanation of the two chemotherapy options. I wonder why the initial U.S. study wasn’t an exact duplicate of the Japanese one, given their results?
Among those who achieve longer-than-average remissions, have there been any studies on the distinguishing traits or habits of these survivors?
And if I haven’t asked too many questions yet, is chemotherapy the only type of new treatment being studied for extensive SCLC?
teriw
Teri,
The two US trials with cisplatin and irinotecan were planned to answer related but slightly different questions. The industry-sponsored one that has been reported by Hanna and colleagues as essentially showing similar results for both options was designed to test whether there was an easier and more feasible way to give cisplatin and irinotecan than the way that was used in the Japanese trial. It used lower doses of cisplatin given two weeks in a row instead of a big slug on one day (which has many more side effects than lower doses over more days) and gave the irinotecan over two weekly doses instead of three, as was done in Japan. In Japan, they couldn’t give that third week of irinotecan about 50% of the time, because patients had low counts. So when the first US-based trial showed no real difference in survival, that could be because of any of three possibilities:
1) there really are no differences, and the Japanese study was a fluke
2) there really are differences among Japanese patients, but in a more heterogeneous US population, drugs work differently, and cisplatin/irinotecan is not as relatively beneficial
3) there really is a benefit to cisplatin/irinotecan, but by changing the doses and schedules in the first trial, we lost that benefit
So the SWOG trial that is being completed will clarify whether scenario #3 is the case. If it’s just that the first trial changed too many variables, this trial will keep all of the variables the same except for using US doctors and US patients. If negative, we will need to debate whether it’s because there really are no differences between these regimens or whether you can have different truths in the US and Japan (and it’s looking like that may be the case with other chemo regiments, due to genetic differences).
Otherwise, there have been no studies yet to discriminate clinical or behavioral features of patients who do especially well vs. poorly with SCLC treatment.
And I’ll write a future post or two about targeted therapies for SCLC. The short answer is that none of these has panned out in early studies.
Thanks for your interest.
-Dr. West
Dr. West -
The doctors are talking of some recent study that says phalidimide (spelling?),a drug that was taken off the market in the 1960’s for causing birth defects, and how it prolongs the regeneration of SCLC cells from regenerating. I am wondering what “prolong” really means. I am sure it depends on each patient, but would like to know more. Have you heard about this or do you know where I can look it up?
Appreciate the help.
Forsyth
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