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Reponses to Topoisomerase-I Inhibitors in Extensive Small-Cell Lung Cancer: Chance or Chromosomes?

University of Missouri/Ellis Fischel Cancer Center, Columbia, MO

For a cancer that is widely regarded as exquisitely sensitive to both radiation therapy and chemotherapy, we seem to have reached a plateau in the treatment of small-cell lung cancer, and no significant advances have seen in extensive-stage disease for several decades. The 2002 article¹ from the Japan Clinical Oncology Group (JCOG) that found the combination of irinotecan and cisplatin to be superior to the standard regimen of etoposide and cisplatin was the first positive news on this front in some time and set off two parallel phenomena. One group of physicians, perhaps frustrated by the therapy they knew, quickly switched to the new combination. Others began to perform comparable trials to see whether the JCOG results could be duplicated in a US population, recalling previous disappointing US trials of agents more successful in Japan (mitomycin, bleomycin, and tegafur and uracil). Two such comparison trials have been completed, and a third, led by the Southwest Oncology Group, has enrolled 470 of a projected 620 patients without unexpected toxicities (R. Natale, personal communication, January 2006). This study uses the same chemotherapy regimens of the JCOG study but not the random assignment to subsequent thoracic radiation therapy.

The topoisomerase-I drugs are particularly intriguing because of their synergism in preclinical studies. Topoisomerase-I drugs may inhibit repair of DNA damage produced by platinating agents and seem like ideal partners for doublet therapy in small-cell lung cancer.²

The JCOG planned to enroll 230 patients, but enrollment was halted because an interim analysis found a statistically meaningful difference in survival between the two groups; a total of only 154 patients, who were evenly split between the two groups, was enrolled (Table 1). Although the differences for progression-free and median survival were significantly in favor of the irinotecan/cisplatin arm (experimental arm), the complete response rate was higher in the etoposide/cisplatin arm, and the 1- and 2-year survival statistics were not statistically significant. Furthermore, the study was restricted to patients less than 70 years of age with good performance scores. The second random assignment to thoracic radiation was not completed. The following question was thus posed: is this a new standard of care?

Eckhardt et al⁴ evaluated the role of oral topotecan in combination with cisplatin. Topotecan is also a camptothecin and a topoisomerase-I inhibitor and, in the intravenous form, is US Food and Drug Administration approved for second-line therapy for small-cell lung cancer. In a multinational, randomized, controlled trial, Eckhardt et al⁴ randomly assigned 784 patients to either oral topotecan for 5 days with intravenous cisplatin on day 1 or intravenous etoposide/cisplatin in a standard regimen. Part of their rationale for this program was the observation that protracted drug exposure may produce greater topoisomerase-I–DNA complex formation and superior cytotoxicity. They found no difference in overall survival, the primary end point, between the two groups. Although they expressed survival in weeks, not months, their survival statistics were similar to the 10 months seen in the other trials, except for the one arm of the JCOG study. Response rates and 1-year survival were also not different between the two groups. Toxicity was felt to be tolerable in both arms, and there were no important differences in Lung Cancer Symptom Scores.

So, at this point in time, we have been unable, in both US and international patients, to duplicate the results of Noda et al.¹ Is this a random, statistical fluke, the one in 20 studies that goes against the grain, or does this represent a genuine difference? Although there are clear differences in trial design and drug dosing, these seem unlikely to account for the differences. One place to look is the obvious possibility of pharmacogenetic differences between a fairly homogenous Japanese population and the much more heterogeneous US and European populations. The Southwest Oncology Group study, which looks at the ability to use genetic markers to predict toxicity and clinical outcomes, may answer this question.

Meanwhile, what are the alternatives? We already know that the addition of a third active agent, paclitaxel, to etoposide and cisplatin improves response rates but not median survival at the expense of increased toxicity.⁵ In an editorial accompanying the Noda et al¹ article, Carney argues that prevention, early detection, and the use of specific biologic targets may be valid alternatives to the further pursuit of "nonspecific, nonselective, and toxic" therapy.⁶ He may be right.

Author's Disclosures of Potential Conflicts of Interest

The author indicated no potential conflicts of interest.

Author Contributions

Manuscript writing: Michael C. Perry

 

REFERENCES

1. Noda K, Nishiwaki Y, Kawahara M, et al: Irinotecan plus cisplatin compared with etoposide plus cisplatin for extensive small cell-lung cancer. N Engl J Med 346:85-91, 2002[Abstract/Free Full Text]

2. Rowinsky EK, Kaufmann SH: Topotecan in combination chemotherapy. Semin Oncol 24:S20-11–S20-26, 1997 (suppl 6)

3. Hanna, N, Bunn P, Langer, et al: Randomized, phase III trial comparing irinotecan/cisplatin with etoposide/cisplatin in patients with previously untreated, extensive-stage disease, small-cell lung cancer. J Clin Oncol 24:2038-2043, 2006[Abstract/Free Full Text]

4. Eckhardt JR, von Pawel J, Papai Z, et al: An open-label, multicenter, randomized, phase III study comparing oral topotecan/cisplatin versus etoposide/cisplatin as treatment for chemotherapy-naïve patients with extensive-disease small-cell lung cancer. J Clin Oncol 24:2044-2051, 2006[Abstract/Free Full Text]

5. Neill HB, Herndon JE II, Miller AAA, et al: Randomized phase III intergroup trial of etoposide and cisplatin with or without paclitaxel and granulocyte colony-stimulating factors in patients with extensive-stage small-cell lung cancer: Cancer and Leukemia Group Trial 9732. J Clin Oncol 23:3752-3759, 2005[Abstract/Free Full Text]

6. Carney DN: Lung cancer: Time to move on from chemotherapy. N Engl J Med 346:126-128, 2002[Free Full Text]

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