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Cancer Research and Treatment > Volume 44(1); 2012 > Article
Saijo: Present Status and Problems on Molecular Targeted Therapy of Cancer

Abstract

Numerous clinical trials of molecular targeted drugs for cancer have been conducted, with remarkable results for certain drugs and accumulation of "negative data" causing a hitch in the development plan for some other compounds. Five recent issues and problems of molecular targeted therapies were discussed critically. Drug discovery and effects against driver mutations (activating mutations) and problems: possibility for circumventing inherent and acquired resistance with the aim of achieving radical cure. Synthetic lethality: reasonable patient selection in individualized treatment strategy. Response rate and progression-free survival improvement with or without overall survival benefit and enhancement of toxicity in bevacizumab therapy: best endpoints for the evaluation of effect of antiangiogenic therapy. Negative data on small-molecule targeted therapy, primarily vascular endothelial growth factor tyrosine kinase inhibitors: loose GO or NO-GO decision criteria for further development of new compounds in early clinical trials. Effect of immunotherapy: difficulty to verify by proof of principle study. We are faced to many questions for the development of efficient personalized therapy. Accumulation of scientific global preclinical and clinical evidences is essential to use these new therapeutic modalities for the improvement of oncologic health care.

Drug Discovery, against Driver Mutations(Activating Mutation) Effects and Problems

Drugs against small-molecule substances and antibodies which specifically control genes serving as a driving force for cancer growth, called activated mutant gene, have been demonstrated to afford the most distinct beneficial effect among the molecular target drugs currently under investigation [1]. This is because growth of cancer is dependent solely on the mutant genes.
These molecular targeted drugs include imatinib directed against breakpoint cluster region-abelson (BCR-ABL) for chronic myeloid leukemia (CML), imatinib directed against mutant c-kit for gastrointestinal stromal tumor (GIST), erlotinib and gefinitib directed against mutant epidermal growth factor receptor (EGFR) for non-small cell lung cancer (NSCLC), crizotinib directed against echinoderm microtubule-associated protein-like 4-anaplastic lymphoma kinase (EML4-ALK) for NSCLC, and vemurafenib directed against mutant B-type Raf kinase (BRAF) for melanoma. All of these drugs have been demonstrated to yield high response rates and to significantly prolong the disease-free survival, progression-free-survival (PFS) and overall survival (OS) when administered alone, and are hence generally accepted as standard treatments for the relevant disorders (Table 1) [2,3].
One of the issues needings to be explored is that while a significant prolongation of OS was demonstrated for imatinib and vemurafenib in randomized comparative studies with cytotoxic anticancer agents, no such prolongation of OS has been demonstrated for gefinitib or erlotinib in spite of their dramatic antitumor activity. Such discrepant results may be attributable to the molecular target drugs being administered to virtually all patients in the chemotherapy-treated group in a crossover design after the disease has progressed. In fact, a comparative study of vemurafenib versus dacarbazine (DTIC) conducted in patients with advanced melanoma using a protocol that prohibited crossover medications demonstrated a significantly prolonged OS in the vemurafenib-treated group (Table 2) [4]. This study design was called into question by The New York Times and other media in the United States from the ethical viewpoint (Fig. 1) [5]. However, such a study design is perhaps acceptable under circumstances where it is uncertain whether a drug actually produces a theoretically anticipated effect or not. In cases for gefinitib and erlotinib, on the other hand, various clinical trials were conducted at the outset of the clinical development of these drugs under the assumption that the target might be wild-type EGFR, and it became evident that patient populations with such clinical characteristics as adenocarcinomas, non-smokers and females were likely to benefit to some extent from the targeted therapies. In April and May, 2004, it was reported that the true target of these drugs was a mutant EGFR [6,7]. Under such a situation, it became extremely difficult to prohibit a crossover design in comparative studies in patients bearing mutant EGFR due to ethical reason.
Second problem will be frequency of each driver mutation. BCR-ABL gene translocation is noted in practically all CML patients. c-kit mutation in GIST, in which cases imatinib is effective, EGFR mutation in NSCLC, and BRAF mutation in melanoma are detected in considerable proportion such as > 90%, about 10-35%, and 40-60%, respectively of the patients [8-10]. On the other hand, the EML4-ALK fusion gene in NSCLC is found in only about 4% of patients with adenocarcinoma of the lung [11]. The frequency of the BRAF mutation in NSCLC is ≤2% [12]. If different driver mutations were discovered in only small fractions of patients in the future, individualized drug discovery and selection of patients may possibly become more and more complicated. Another important problem to be tackled will be up to what extent of market size contraction the researchers'/firm's will to discover drugs can be maintained.
Third issue will be circumvention of drug resistance to each drug. These therapeutic agents produce dramatic effects in most patients at the beginning of the treatment, however, there are some patients who do not respond at all even in the presence of a driver mutation (Resistance 1). It has been pointed out that this could be attributable to the problem in low specificity for the detection of mutations. Even among responders, the majority of patients may fail to achieve complete response, but still show partial response (Resistance 2). Furthermore, occurrence of secondary mutations, such as threonine 790 methionine (T790M) in mutant EGFR, and emergence of resistance through other mechanisms such as activation of another signal transduction pathways are also encountered (Resistance 3). Secondary mutations have also been reported in lung cancer with EML4-ALK fusion gene [13,14]. It is yet to be clarified in regard to Resistance 3, whether the secondary mutation may actually be induced by a drug or represents the result of selection of a sensitive cell population that responds to the drug (Table 3). In any event, radical cure cannot be expected even with sharply acting molecular targeted drugs, unless Resistances 1, 2 and 3 can be circumvented. It is considered an important future subject of research for clinicians to design appropriate combinations of molecular targeted drugs and cytotoxic chemotherapy or combinations of different molecular-targeted drugs. Comparative studies of EGFR-tyrosine kinase inhibitor (TKI)±cytotoxic chemotherapy regimens in non-selected cases of NSCLC have failed to confirm an add-on effect of EGFR-TKI, however, there is still the hope that improved efficacy might be obtained with such therapy in EGFR mutation-positive cases by this strategy. Because median survival time of EGFR-mutation positive patients improved to 27-30 months after the beginning of treatment by the sequential combination of EGFR-TKI+cytotoxic drugs. A recent report described that irreversible EGFR-TKI+cetuximab was effective in EGFR mutation-positive patients who were no longer responsive to erlotinib or gefinitib. There is great hope, of course, that drugs capable of circumventing emergence of resistance will be discovered via elucidation of the underlying mechanisms [15,16].

Patient Selection in a Synthetic Lethality Strategy

Synthetic lethality is a newly-coined term and has been used, for example, to explain how poly ADR-ribose polymerase (PARP) inhibitors are effective only in breast cancer susceptibility gene (BRCA) 1/2 mutation-positive cases [17]. PARP plays an important role in repairing single-stranded DNA cleavage at the sites of DNA damage caused by anticancer agents or radiation. Following administration of PARP inhibitors, the damaged DNA cannot be repaired, leading to accumulation of single-stranded DNA breaks which eventually result in double-stranded DNA breaks. Damaged DNA can be repaired by homologous recombination in cells with normal BRCA1/2, whereas in BRCA1/2-defective cells, no such repair of DNA damage is possible, resulting in cellular death [18-20]. Patients with ovarian cancer or breast cancer with BRCA 1/2 mutation/defect have been reported, and clinical studies of profound interest aimed at synthetic lethality are ongoing (Fig. 2) [18,19,21].
A comparative phase II clinical trial was conducted to assess maintenance therapy with olaparib (PARP inhibitor) in BRCA 1/2 mutation-positive patients after induction chemotherapy for advanced ovarian carcinoma. The study population comprised patients who had received two or more combination chemotherapy regimens including platinum. Although the study was a phase II trial, the results showed significant prolongation of the PFS (p < 0.00001) in patients treated with olaparib as a maintenance therapy [22]. The results of the phase II study performed in 265 patients with sensitive relapse encouraged to do next phase III study.
Triple-negative breast cancer (TNBC) bears similarity to hereditary BRCA1/2 mutation-positive breast cancer with respect to characteristics such as the estrogen-receptor/progesterone receptor/human epidermal growth factor receptor type 2 (ER/PR/HER2) status, p53 status, mutant-type gene expression pattern (basal like), histologic type (poorly differentiated), and sensitivity to DNA-damaging anticancer agents (highly sensitive). Diminished expression of BRCA1/2 is also noted. TNBC has been recognized to have a distribution which overlaps in part with that of BRCA1/2 mutation (defect)-positive breast cancer.
O'Shaughnessy et al. [23] conducted a comparative phase II study of gemcitabine+carboplatin±iniparib in 120 patients with TNBC and published the results in the New England Journal of Medicine. The iniparib add-on group showed both superior PFS and OS in this phase II trial (Fig. 3). With the aim of confirming the outcome, a phase III trial was undertaken in 519 previously treated patients with TNBC, using PFS and OS as the primary endpoints. The trial seemed a highly hopeful comparative study in which 519 TNBC patients were enrolled within a period of as short as 9 months from July 2009 to March 2010. The target number of recruited patients was set at 420 before starting the trial, with hazard ratios of 0.66 and 0.65 for OS and PFS, respectively, and α-error levels of 0.04 and 0.01, respectively, based on a previous phase II trial which had demonstrated an add-on effect of the PARP inhibitor. In the phase III study, however, the hazard ratios for OS and PFS were 0.88 and 0.79, respectively, with p-values of 0.28 and 0.027; hence neither endpoint cleared the estimated value, yielding negative data [24]. The results were one of the most disappointing among those of clinical studies on molecular targeted drugs reported in 2011 (Table 4) [24]. Most probable explanation for the disappointing data may be confusion of the concept of BRCA1/2 mutation (defect) with that of BRCA-ness. The background for the study population consisting of TNBC patients in clinical trials using a PARP inhibitor is based on the hypothesis of BRCA-ness that the BRCA1 promoter is methylated or the BRCA1 function is depressed in TNBC. In other words, mutation/defect of BRCA1/2 and BRCA-ness are entirely different concepts. As can be seen in the Fig. 4, TNBC, basal-like breast cancer (BC) and BRCA1-mutant or defective BC overlap for a considerable part, but BRCA1-mutant or defective BC may constitutes a small proportion of TNBC and basal-like BC [25]. Although, in the phase III trial, clinical characteristics in PR/ER/HER2-negative cases of TNBC were assessed, whereas there were no data concerning the BRCA1/2 status, it would be possible to infer that the proportion of BRCA1/2-mutant (defective) BC cases in the population enrolled in the phase II and III studies affected the study results. Thus, effects of the treatment cannot be expected in studies involving contradiction between the patient inclusion criteria and the target for the molecular targeted drugs. This suggests the cardinal importance of appropriate patient selection based on reliable biomarkers.

Response Rate and PFS Improvement with/without OS Prolongation and Enhancement of Toxicity of Bevacizumab (BEV) Therapy

Angiogenesis inhibitors have been evaluated in clinical studies on a variety of malignancies because they are considered to be non-organ-specific from the viewpoint of efficacy, in as much as angiogenesis inhibitors exert their effects on the cancer milieu rather than on the cancer cells per se. Biomarkers to estimate therapeutic responses, if present at all, cannot be used for a qualitative estimation of the responses to angiogenesis inhibitors in terms of a 'yes' or 'no.' Several comparative studies of BEV have been conducted, which have generated data indicating that while the response rate and PFS improved, there was still no significant improvement of the OS following BEV therapy combined with chemotherapy in most instances (Tables 5 and 6) [26]. Prolongation of OS occurred only in colorectal cancer, following use of BEV in combination with irinote can/fluorouracil/leucovorin or oxaliplatin/fluorouracil/leucovorin (FOLFOX) therapy and paclitaxel+carboplatin regimens for non-small cell carcinoma. In all studies including E2100 [28,42], BEV and Docetaxel (AVADO) [29] and Regimens in Bevacizumab for Breast Oncology (RIBBON) [30,43] trials conducted in patients with advanced BC, only the response rate and PFS improved, with no significant prolongation of the OS, therefore, cancellation of the accelerated approval on the basis of the E2100 trial data has been decided in United States Food and Drug Administration (US FDA) based on Oncology Drug Advisory Committee (ODAC) recommendation (Table 7). Similar results were obtained in the Gynecologic Oncology Group (GOG) 0218 [39], a randomized, double blinded, placebo-controlled, Phase III trial of chemotherapy with or without bevacizumab in patients with platinum sensitive recurrent epithelial ovarian, primary peritoneal or fallopian, tube cancer (OCEANS) [41] and a randomized, two arm, multicenter Gynecologic Cancer InterGroup trial of adding bevacizumab to standard chemotherapy (ICON7) [40] studies conducted in patients with ovarian cancer. A comparative phase II trial was performed in lung cancer in Japan using the same schedule as that in the E4599 study and this trial failed to demonstrate any significant improvement of the OS in the BEV treatment group. Possible reasons for these failures may include 1) the problem of bias in evaluating the PFS, namely, the PFS in the BEV-treated group merely appeared to be better at a glance due to observation bias; 2) an insufficient degree of improvement for antitumor effect of the chemotherapy prescribed concomitantly with BEV; and 3) alterations of the biological characteristics of the residual tumor after combined treatment with BEV-chemotherapy, which may cause the malignant cancer cells to survive and proliferate rapidly in spite of continued treatment. Issues that need to be investigated in relation to the use of BEV may include 1) validity of continued use of BEV even after completion of chemotherapy in combined treatment with chemotherapy; 2) non-negligible adverse reactions that are observed even after exclusion of high-risk patients; 3) high drug prices (Fig. 5); and 4) limited degree of efficacy. BEV is prescribed in only about 10 to 20% of patients, even in the United States, where it is approved for use in the treatment of non-small-cell carcinoma of the lung, therefore, the propriety of the use of BEV should be judged after sufficient analysis of various factors.

Accumulating Negative Data on Small-Molecule Kinase Inhibitors: Loose GO or NO-GO Decision Criteria on Further Development of New Compounds

Numerous studies for the development of small-molecule kinase (SMK) inhibitors are currently in progress. Among the most prominent SMK inhibitors that are under development are the multitargeted kinase inhibitors, targeting mainly on vascular endothelial growth factor receptor. Such multitargeted SMK inhibitors as sunitinib and sorafenib have been already in the market and are used as therapeutic agents renal cancer and hepatoma, but the precise mechanism of antitumor effect of these drugs remains unclear. The results of many clinical studies on SMK inhibitors under development have yielded negative data. The reason thereof may be said to be a mistake based on loose criteria for the GO or NO-GO decision about proceeding from non-clinical studies to clinical trials and from early-phase clinical trials to phase III trials [26]. It seems often the case that the magnitude of the antitumor effect is misjudged for data of non clinical studies. The non-clinical study data which have come to our notice are largely favorable and purport to demonstrate theoretically tenable antitumor effects. We must not disregard the possibility that there actually exists a vast amount of negative data underneath of positive results. On the other hand, insufficiently explained positive data also exist, and in some cases, an effect on a target distinct from an initially anticipated target is ultimately linked with the observed therapeutic effect. Designs of early phase clinical trials and interpretation of proof of principle (POP) data also have great influence on the GO/NO-GO decision preceding a big scale phase III trial. It is also an important subject as to which of the hitherto obtained study data recognized as global standards can be considered as reliable. Gefitinib and erlotinib are thought to be first-line drugs for the treatment of non-small-cell carcinoma expressing EGFR mutations; however, strangely, patient selection is generally considered unnecessary while prescribing erlotinib, as second-line treatment. Erlotinib has been strangely believed to be active even for patients without EGFR mutation in western investigators based on the results of BR-21 study [44]. On the other hand, gefitinib is considered to be inactive based on the results of IRESSAPan Asia Study (IPASS) trial [45] in n spite of the statistical demonstration for non-inferiority of gefitinib in Gefitinib and docetaxel trial in previously treated non-small cell lung cancer (INTEREST) study [46]. It would also be a future important subject to explore the validity of assessing the add-on effect of a new SMK inhibitor in a phase III comparative study of second-line and third-line regimens using erlotinib [47] in a comparator group in non-selected patients with non-small-cell carcinoma. It can be readily assumed that a comparative study of a multitargeted SMK inhibitor with or without a concomitant merely cytotoxic anticancer agent with the anticancer agent alone will yield negative data if tumor shrinkage may not be expected from monotherapy with the multitargeted SMK inhibitor directed towards mutations other than the driver mutation. This is simply because add-on effect can hardly be expected from a compound with only a small degree of antitumor effect.

Effect of Immunotherapy nearly Impossible to Verify by a POP Study

Immunotherapy was once regarded as a dubious treatment. Although the underlying mechanism of action can be cogently described, it is too complex and nearly impossible to verify through POP studies. There is no other means than demonstrating an overwhelming therapeutic effect of immunotherapy in scientific clinical studies to convince researchers, regulatory authorities and patients, in particular, under such circumstances. Recently, positive data on immunotherapy have been reported sporadically seen in the literature. Manufacture of Sipuleucel-T has been approved by the US FDA. Sipuleucel-T is a treatment consisting of injection of autologous peripheral blood dendritic cells, cultured in the presence of PA2024, a fusion protein composed of prostatic acid phosphatase (PAP) linked to granulocyte-macrophage colony-stimulating factor, which is an activated immune cell preparation targeted against PAP antigen. This complicated therapy was evaluated in a randomized placebo-controlled double-blind trial in 1,512 patients with asymptomatic, metastasis-positive, non-androgen-dependent cancer of the prostate (IMPACT Study). The mean survival time was 25.8 months in the Sipuleucel-T therapy group, as compared to 21.7 months in the placebo group (p=0.017); hence, the outcome was superior in the former [48], and the therapy was approved by the FDA on April 29, 2010, based on these results. This is a first approval of immunotherapy in US FDA.
At the 2010 American Society of Clinical Oncology (ASCO) Annual Meeting, a three-group parallel trial of the following three treatment groups, namely, ipilimumab+gp100, ipilimumab+placebo and gp100+placebo, in previously treated patients with malignant melanoma (molecular diagnostics [MDX] 010-20 Study) was reported. Gp100 antigen is expressed in the majority of melanoma cells. It has been reported that the cytotoxic T-lymphocyte antigen (CTLA)-4 on T cells inhibits binding of cluster of differentiation 28 (CD28) to B7 on the T cells by binding B7 on antigen presentation cells, thereby suppressing T cell activation (Fig. 6). It has been speculated that the binding of CD28 to B7 becomes possible when CTLA-4 is blocked by ipilimumab, resulting in T cell activation, and its function becomes enhanced. In the MDX010-20 Study with the primary endpoint consisting of assessments of the prolonging effects for OS of the ipilimumab+gp100 group (Arm A) and gp100 (Arm C) as the positive control group, the study was designed to also enable comparison of the gp100 group and an ipilimumab group (Arm B) (Table 8). Results of the study showed that the results in Arms A and B were significantly superior in terms of the OS than in Arm C. There was no significant difference between Arms A and B in the OS, although it was a little bit better in Arm B [49]. At the 2011 ASCO Annual Meeting, a randomized comparative trial to evaluate the add-on effect of ipilimumab to dacarbazine (DTIC), which is the standard treatment for previously untreated melanoma was reported. The combined therapy of ipilimumab and DTIC group showed superior OS (hazard ratio, 0.72; p=0.0009), PFS and duration of sustained response (Table 9) [50]. It seems very likely that this combination therapy will become the standard treatment for melanomas, and studies may probably generate results of various assessments of this treatment as adjuvant therapy.
Ipilimumab is an antibody to CTLA-4 and works by restoring T cell activity. It has the effect of indirectly potentiating immunity, yet the effect is non-specific. It is considered an important problem to deal with how POP studies should be conducted in the case of such a compound. Rapid improvement of therapeutic responses using combined vemurafenib plus ipilimumab therapy for BRAF V600E mutation positive melanoma is expected.

Conclusion

Five topics pertaining to the effects and problems of the currently available molecular targeted therapies for malignancies have been reviewed critically. Personalized cancer therapy using molecular targeted drugs have just integrated in clinical practice, however, majority of cancer patients still cannot be cured. Beside, molecular targeted therapies show more than minimal problems including patient selection, drug induced adverse events and high costs. Physicians should make an effort to be fully aware of these problems and to devote for research and medical practice to improve oncologic medical care.

Conflicts of Interest

Conflict of interest relevant to this article was not reported.

References

1. Weinstein IB, Joe AK. Mechanisms of disease: oncogene addiction-a rationale for molecular targeting in cancer therapy. Nat Clin Pract Oncol. 2006;3:448–457. PMID: 16894390
crossref pmid
2. Jackman DM, Miller VA, Cioffredi LA, Yeap BY, Jänne PA, Riely GJ, et al. Impact of epidermal growth factor receptor and KRAS mutations on clinical outcomes in previously untreated non-small cell lung cancer patients: results of an online tumor registry of clinical trials. Clin Cancer Res. 2009;15:5267–5273. PMID: 19671843
crossref pmid pmc
3. Kwak EL, Bang YJ, Camidge DR, Shaw AT, Solomon B, Maki RG, et al. Anaplastic lymphoma kinase inhibition in non-small-cell lung cancer. N Engl J Med. 2010;363:1693–1703. PMID: 20979469
crossref pmid pmc
4. Chapman PB, Hauschild A, Robert C, Larkin JM, Haanen JB, Ribas A, et al. Phase III randomized open label, multicenter trial (BRIM3) comparing BRAF inhibitor vemurafenib with dacarbazine (DTIC) in patients with V600EBRAF-mutated melanoma. J Clin Oncol. 2011;29(S):LBA4.
crossref
5. CTV News: Vemurafenib in melanoma: was its phase 3 trial unethical? [Internet]. cited 2011 Dec 20Scarborough, ON: CTV Television Network; Available from: http://healthblog.ctv.ca

6. Paez JG, Jänne PA, Lee JC, Tracy S, Greulich H, Gabriel S, et al. EGFR mutations in lung cancer: correlation with clinical response to gefitinib therapy. Science. 2004;304:1497–1500. PMID: 15118125
crossref pmid
7. Lynch TJ, Bell DW, Sordella R, Gurubhagavatula S, Okimoto RA, Brannigan BW, et al. Activating mutations in the epidermal growth factor receptor underlying responsiveness of non-small-cell lung cancer to gefitinib. N Engl J Med. 2004;350:2129–2139. PMID: 15118073
crossref pmid
8. Siehl J, Thiel E. C-kit, GIST, and imatinib. Recent Results Cancer Res. 2007;176:145–151. PMID: 17607922
crossref pmid
9. Mitsudomi T, Yatabe Y. Mutations of the epidermal growth factor receptor gene and related genes as determinants of epidermal growth factor receptor tyrosine kinase inhibitors sensitivity in lung cancer. Cancer Sci. 2007;98:1817–1824. PMID: 17888036
crossref pmid
10. Flaherty KT, Puzanov I, Kim KB, Ribas A, McArthur GA, Sosman JA, et al. Inhibition of mutated, activated BRAF in metastatic melanoma. N Engl J Med. 2010;363:809–819. PMID: 20818844
crossref pmid pmc
11. Soda M, Choi YL, Enomoto M, Takada S, Yamashita Y, Ishikawa S, et al. Identification of the transforming EML4-ALK fusion gene in non-small-cell lung cancer. Nature. 2007;448:561–566. PMID: 17625570
crossref pmid
12. Marchetti A, Felicioni L, Malatesta S, Grazia Sciarrotta M, Guetti L, Chella A, et al. Clinical features and outcome of patients with non-small-cell lung cancer harboring BRAF mutations. J Clin Oncol. 2011;29:3574–3579. PMID: 21825258
crossref pmid
13. Choi YL, Soda M, Yamashita Y, Ueno T, Takashima J, Nakajima T, et al. EML4-ALK mutations in lung cancer that confer resistance to ALK inhibitors. N Engl J Med. 2010;363:1734–1739. PMID: 20979473
crossref pmid
14. Sasaki T, Koivunen J, Ogino A, Yanagita M, Nikiforow S, Zheng W, et al. A novel ALK secondary mutation and EGFR signaling cause resistance to ALK kinase inhibitors. Cancer Res. 2011;71:6051–6060. PMID: 21791641
crossref pmid pmc
15. Saijo N. Critical comments for roles of biomarkers in the diagnosis and treatment of cancer. Cancer Treat Rev. 2012;38:63–67. PMID: 21652149
crossref pmid
16. Sequist LV, Waltman BA, Dias-Santagata D, Digumarthy S, Turke AB, Fidias P, et al. Genotypic and histological evolution of lung cancers acquiring resistance to EGFR inhibitors. Sci Transl Med. 2011;3:75ra26.
crossref pmid pmc
17. Rehman FL, Lord CJ, Ashworth A. Synthetic lethal approaches to breast cancer therapy. Nat Rev Clin Oncol. 2010;7:718–724. PMID: 20956981
crossref pmid
18. Farmer H, McCabe N, Lord CJ, Tutt AN, Johnson DA, Richardson TB, et al. Targeting the DNA repair defect in BRCA mutant cells as a therapeutic strategy. Nature. 2005;434:917–921. PMID: 15829967
crossref pmid
19. Bryant HE, Schultz N, Thomas HD, Parker KM, Flower D, Lopez E, et al. Specific killing of BRCA2-deficient tumours with inhibitors of poly(ADP-ribose) polymerase. Nature. 2005;434:913–917. PMID: 15829966
crossref pmid
20. McCabe N, Lord CJ, Tutt AN, Martin NM, Smith GC, Ashworth A. BRCA2-deficient CAPAN-1 cells are extremely sensitive to the inhibition of Poly (ADP-Ribose) polymerase: an issue of potency. Cancer Biol Ther. 2005;4:934–936. PMID: 16251802
crossref pmid
21. McCabe N, Turner NC, Lord CJ, Kluzek K, Bialkowska A, Swift S, et al. Deficiency in the repair of DNA damage by homologous recombination and sensitivity to poly(ADP-ribose) polymerase inhibition. Cancer Res. 2006;66:8109–8115. PMID: 16912188
crossref pmid
22. Ledermann JA, Harter P, Gourley C, Friedlnder M, Vergote IB, Rustin GJ, et al. Phase II randomized placebo-controlled study of olaparib (AZD2281) in patients with platinum-sensitive relapsed serious ovarian cancer (PSR SOC). J Clin Oncol. 2011;29(S):5003.
crossref
23. O'Shaughnessy J, Osborne C, Pippen JE, Yoffe M, Patt D, Rocha C, et al. Iniparib plus chemotherapy in metastatic triple-negative breast cancer. N Engl J Med. 2011;364:205–214. PMID: 21208101
crossref pmid
24. O'Shaughnessy J, Schwartzberg LS, Danso MA, Rugo HS, Miler K, Yardly DA, et al. A randomized phase III study of iniparib (BSI-201) in combination with gemcitabine/carboplatin (G/C) in metastatic triple-negative breast cancer (TNBC). J Clin Oncol. 2011;29(S):1007PMID: 21205758
crossref pmid pmc
25. Pal SK, Childs BH, Pegram M. Triple negative breast cancer: unmet medical needs. Breast Cancer Res Treat. 2011;125:627–636. PMID: 21161370
crossref pmid pmc
26. Saijo N. Problems involved in the clinical trials for non-small cell lung carcinoma. Cancer Treat Rev. 2012;2011 Jul 19 [Epub] http://dx.doi.org/10.1016/j.ctrv.2011.06.001
crossref
27. Miller KD, Chap LI, Holmes FA, Cobleigh MA, Marcom PK, Fehrenbacher L, et al. Randomized phase III trial of capecitabine compared with bevacizumab plus capecitabine in patients with previously treated metastatic breast cancer. J Clin Oncol. 2005;23:792–799. PMID: 15681523
crossref pmid
28. Miller K, Wang M, Gralow J, Dickler M, Cobleigh M, Perez EA, et al. Paclitaxel plus bevacizumab versus paclitaxel alone for metastatic breast cancer. N Engl J Med. 2007;357:2666–2676. PMID: 18160686
crossref pmid
29. Miles DW, Chan A, Dirix LY, Cortés J, Pivot X, Tomczak P, et al. Phase III study of bevacizumab plus docetaxel compared with placebo plus docetaxel for the first-line treatment of human epidermal growth factor receptor 2-negative metastatic breast cancer. J Clin Oncol. 2010;28:3239–3247. PMID: 20498403
crossref pmid
30. Robert NJ, Diéras V, Glaspy J, Brufsky AM, Bondarenko I, Lipatov ON, et al. RIBBON-1: randomized, double-blind, placebo-controlled, phase III trial of chemotherapy with or without bevacizumab for first-line treatment of human epidermal growth factor receptor 2-negative, locally recurrent or metastatic breast cancer. J Clin Oncol. 2011;29:1252–1260. PMID: 21383283
crossref pmid
31. Meyerhardt JA, Mayer RJ. Systemic therapy for colorectal cancer. N Engl J Med. 2005;352:476–487. PMID: 15689586
crossref pmid
32. Hurwitz HI, Fehrenbacher L, Hainsworth JD, Heim W, Berlin J, Holmgren E, et al. Bevacizumab in combination with fluorouracil and leucovorin: an active regimen for first-line metastatic colorectal cancer. J Clin Oncol. 2005;23:3502–3508. PMID: 15908660
crossref pmid
33. Saltz LB, Clarke S, Díaz-Rubio E, Scheithauer W, Figer A, Wong R, et al. Bevacizumab in combination with oxaliplatin-based chemotherapy as first-line therapy in metastatic colorectal cancer: a randomized phase III study. J Clin Oncol. 2008;26:2013–2019. PMID: 18421054
crossref pmid
34. Allegra CJ, Yothers G, O'Connell MJ, Sharif S, Colangelo LH, Lopa SH, et al. Initial safety report of NSABP C-08: A randomized phase III study of modified FOLFOX6 with or without bevacizumab for the adjuvant treatment of patients with stage II or III colon cancer. J Clin Oncol. 2009;27:3385–3390. PMID: 19414665
crossref pmid pmc
35. Sandler A, Gray R, Perry MC, Brahmer J, Schiller JH, Dowlati A, et al. Paclitaxel-carboplatin alone or with bevacizumab for non-small-cell lung cancer. N Engl J Med. 2006;355:2542–2550. PMID: 17167137
crossref pmid
36. Reck M, von Pawel J, Zatloukal P, Ramlau R, Gorbounova V, Hirsh V, et al. Phase III trial of cisplatin plus gemcitabine with either placebo or bevacizumab as first-line therapy for nonsquamous non-small-cell lung cancer: AVAil. J Clin Oncol. 2009;27:1227–1234. PMID: 19188680
crossref pmid
37. Escudier B, Pluzanska A, Koralewski P, Ravaud A, Bracarda S, Szczylik C, et al. Bevacizumab plus interferon alfa-2a for treatment of metastatic renal cell carcinoma: a randomised, double-blind phase III trial. Lancet. 2007;370:2103–2111. PMID: 18156031
crossref pmid
38. Ohtsu A, Shah MA, Van Cutsem E, Rha SY, Sawaki A, Park SR, et al. Bevacizumab in combination with chemotherapy as first-line therapy in advanced gastric cancer: a randomized, double-blind, placebo-controlled phase III study. J Clin Oncol. 2011;29:3968–3976. PMID: 21844504
crossref pmid
39. Burger RA, Brady MF, Bookman MA, Walker JL, Homesley HD, Fowker J, et al. Phase III trial of bevacizumab (BEV) in the primary treatment of advanced epithelial ovarian cancer (EOC), primary peritoneal cancer (PPC), or fallopian tube cancer (FTC): a Gynecologic Oncology Group study. J Clin Oncol. 2010;28(18S):LBA1.
crossref
40. Kristensen G, Perren T, Qian W, Pfisterer J, Ledermann JA, Joly F, et al. Result of interim analysis of overall survival in the GCIG ICON7 phase III randomized trial of bevacizumab in women with newly diagnosed ovarian cancer. J Clin Oncol. 2011;29(S):LBA5006.
crossref
41. Aghajanian C, Finkler NJ, Ruterford T, Smith DA, Yi J, Parmar H, et al. Oceans: a randomized, double-blinded, placebo-controlled phase III trial of chemotherapy with or without bevacizumab in patients with platinum-sensitive recurrent epithelial ovarian, primary peritoncal, or fallopian tube cancer. J Clin Oncol. 2011;29(S):LBA5007.
crossref pmid pmc
42. Gray R, Bhattacharya S, Bowden C, Miller K, Comis RL. Independent review of E2100: a phase III trial of bevacizumab plus paclitaxel versus paclitaxel in women with metastatic breast cancer. J Clin Oncol. 2009;27:4966–4972. PMID: 19720913
crossref pmid pmc
43. Burstein HJ. Bevacizumab for advanced breast cancer: all tied up with a RIBBON? J Clin Oncol. 2011;29:1232–1235. PMID: 21383305
crossref pmid
44. Shepherd FA, Rodrigues Pereira J, Ciuleanu T, Tan EH, Hirsh V, Thongprasert S, et al. Erlotinib in previously treated non-small-cell lung cancer. N Engl J Med. 2005;353:123–132. PMID: 16014882
crossref pmid
45. Mok TS, Wu YL, Thongprasert S, Yang CH, Chu DT, Saijo N, et al. Gefitinib or carboplatin-paclitaxel in pulmonary adenocarcinoma. N Engl J Med. 2009;361:947–957. PMID: 19692680
crossref pmid
46. Kim ES, Hirsh V, Mok T, Socinski MA, Gervais R, Wu YL, et al. Gefitinib versus docetaxel in previously treated non-small-cell lung cancer (INTEREST): a randomised phase III trial. Lancet. 2008;372:1809–1818. PMID: 19027483
crossref pmid
47. Schiller JH, Akerley WL, Brugger W, Ferrari D, Garmey EG, Gerber DE, et al. Results of ARQ 197-209: a global randomized placebo-controlled phase II clinical trial of erlotinib plus ARQ 197 versus erlotinib plus placebo in previously treated EGFR inhibitor-naïve patients with locally advanced metastatic non-small cell lung cancer (NSCLC). J Clin Oncol. 2010;28(18S):LBA7502.
crossref
48. Kantoff PW, Higano CS, Shore ND, Berger ER, Small EJ, Penson DF, et al. Sipuleucel-T immunotherapy for castration-resistant prostate cancer. N Engl J Med. 2010;363:411–422. PMID: 20818862
crossref pmid
49. Hodi FS, O'Day SJ, McDermott DF, Weber RW, Sosman JA, Haanen JB, et al. Improved survival with ipilimumab in patients with metastatic melanoma. N Engl J Med. 2010;363:711–723. PMID: 20525992
crossref pmid pmc
50. Robert C, Thomas L, Bondarenko I, O'Day S, Weber J, Garbe C, et al. Ipilimumab plus dacarbazine for previously untreated metastatic melanoma. N Engl J Med. 2011;364:2517–2526. PMID: 21639810
crossref pmid
Fig. 1
Your Health-CTV Med News Express (From CTV News, Vemurafenib in melanoma: was its phase 3 trial unethical?, with permission from CTV Television Network) [5].
crt-44-1-g001.jpg
Fig. 2
Mechanism for synthetic lethality in BRCA1/2 deficient cancer. Poly ADR-ribose polymerase (PARP) inhibition produces tumor-selective synthetic lethaity. When PARP action is inhibited, SS are converted to DSB at replication. In cells with functional HR pathway, the DSB will be repaired. In cells with a dysfunctional HR pathway, as is the case with BRCA 1 and 2, the lesions go unrepaired and cell death ensues [18,19,21]. BRCA, breast cancer susceptibility gene; DSB, double-strand break; HR, homologous recombination; SSB, single-strand break.
crt-44-1-g002.jpg
Fig. 3
Efficacy of iniparib in triple negative breast cancer progression-free survival/overall survival (phase II study). CI, confidence interval [23].
crt-44-1-g003.jpg
Fig. 4
Schematic illustration of overlap among triple negative breast cancer, basal-like, and BRCA1-related tumors adapted from Pal et al. [25]. BRCA1, breast cancer susceptibility gene.
crt-44-1-g004.jpg
Fig. 5
Increased treatment cost by bevacizumab (Bev). CBDCA, carboplatin; PTL, paclitaxel.
crt-44-1-g005.jpg
Fig. 6
Mode of action of ipilimumab. CTLA-4, cytotoxic T-lymphocyte antigen-4; TCR, T-cell receptor; MHC, major histocompatibility complex; APC, antigen-presenting cell.
crt-44-1-g006.jpg
Table 1
Clinical evidence of oncogene addiction [1]
Target Disease Agent Regimen Response rate (%)
Mutant EGFR NSCLC Gefitinib, erlotinib Monotherapy 70-90
EML4-ALK NSCLC Crizotinib Monotherapy 70-90
BCR/ABL CML Imatinib Monotherapy 70-90
c-KIT GIST Imatinib Monotherapy 45
Mutant BRAF Melanoma Vemurafenib Monotherapy 50

EGFR, epidermal growth factor receptor; NSCLC, non-small cell lung cancer; EML4-ALK, echinoderm microtubule-associated protein-like 4-anaplastic lymphoma kinase; BCR-ABL, breakpoint cluster region-abelson; CML, chronic myeloid leukemia; GIST, gastrointestinal stromal tumor; BRAF, B-type Raf kinase.

Table 2
Comparison of overall survival of unresectable BRAF V600E mutated malignant melanoma treated with dacarbazine vs. vemurafenib (BRIM3 trial) [4]
Dacarbazine Vemurafenib
No. of patients 338 337
Response rate (%) 5.5 48.4
Median progression free survival (M) 1.6 5.3
Hazard ratio, 0.26 (0.20-0.33); p < 0.0001
Overall survival (6 mo survival, %) 64 84
Hazard ratio, 0.37 (0.26-0.55); p < 0.0001
Table 3
Problems for cure by molecular target therapy
1) Wild type tumor
2) Driver mutation positive tumor
 (1) Absolutely refratory tumor
  PD or SD in spite of driver mutation
 (2) Heterogeneity of tumor
  Majority achieve only PR
 (3) Acquired resistance
  Secondary? mutation
  Activation of other pathways (T790M)
   MET amplification
   Activation of HGF mediated pathway
   Transformation of pathological characteristics

PD, progressive disease; SD, stabilized disease; PR, partial response; MET, MNNG HOS transforming gene; HGF, hepatocyte growth factor.

Table 4
Efficacy endpoints for phase III study of iniparib ITT population [24]
GC (n=258) GCI (n=261)
PFS (pre-specified alpha=0.01)
 Median PFS (95% CI, mo) 4.1 (3.1, 4.6) 5.1 (4.2, 5.8)
 HR (95% CI) 0.79 (0.65, 0.98)
 p-value 0.027
OS (pre-specified alpha=0.04)
 Median OS (95% CI, mo) 11.1 (9.2, 12.1) 11.8 (10.6, 12.9)
 HR (95% CI) 0.88 (0.69, 1.12)
 p-value 0.28

ITT, Intent to treat; GC, gemcitabine-carboplatin; GCI, gemcitabine-carboplatin plus iniparib; PFS, progression free survival; CI, confidence interval; HR, hazard ratio; OS, overall survival.

Table 5
Clinical benefit with bevacizumab (BV) in phase III studies: part 1
 Primary site Regimen Publication RR PFS OS
M-BC (R) Capecitabine±BV JCO 2005 [27] × ×
M-BC (E2100) Paclitaxel±BV NEJM 2007 [28] ×
M-BC (AVADO) Docetaxel±BV JCO 2010 [29] ×
M-BC (RIBBON) Anthra/Toxan/Cape±BV JCO 2011 [30] NE ×
M-CRC IFL±BV NEJM 2005 [31] NE
M-CRC (R) FOLFOX±BV JCO 2005 [32] NE NE
M-CRC XELOX/FOLFOX±BV JCO 2008 [33] NE ×
Adjuvant (RC) FOLFOX6±BV JCO 2009 [34] NE × NE

RR, relative risk; PFS, progression-free survival; OS, overall survival; JCO, Journal of Clinical Oncology; NEJM, New England Journal of Medicine; IFL, irinotecan/fluorouracil/leucovorin; FOLFOX, oxaliplatin/fluorouracil/leucovorin; ○, significant; ×, not significant; NE, not evaluable.

Table 6
Clinical benefit with bevacizumab (BV) in phase III studies: part 2
 Primary site Regimen Publication RR PFS OS
M-NSCLC CBDCA+TXL±BV NEJM 2006 [35]
M-NSCLC CDDP+GEM±BV JCO 2009 [36] ×
Renal cell (AVOREN) IFN±BV Lancet 2007 [37] NE ×
Gastric ca (AVAGAST) Cap/FU+CDDP±BV JCO 2011 [38] ×
Ovarian ca (GOG-0218) CBDCA+TXL±BV JCO 2010 [39] NE ×
Ovarian ca (ICON7) CBDCA+TXL±BV JCO 2011 [40] --- ×
Ovarian ca (OCEANS) CBDCA+GEM±BV JCO 2011 [41] ×

RR, response rate; PFS, progression-free survival; OS, overall survival; NSCLC, non-small cell lung cancer; CBDCA, carboplatin; TXL, paclitaxel; NEJM, New England Journal of Medicine; CDDP, cisplatin; GEM, gemcitabine; JCO, Journal of Clinical Oncology; Ca, cancer; AVOREN, Phase III trial of bevacizumab plus interfern alfa-2a in patients with metastatic renal cell carcinoma; IFN, interferon; NE, not evaluable; AVAGAST, a randomized, double-blind, placebo-controlled, phase III study of first-line capecitabine and cisplatin plus bevacizumab or placebo in patients with advanced gastric cancer; GOG, Gynecologic Oncology Group; ICON, a randomized, two arm, multicenter Gynecologic Cancer InterGroup trial of adding bevacizumab to standard chemotherapy; OCEANS, a randomized, double blinded, placebo-controlled, phase III trial of chemotherapy with or without bevacizumab in patients with platinum sensitive recurrent epithelial ovarian, primary peritoneal or fallopian, tube cancer; ○, significant; ×, not significant.

Table 7
Voting results of ODAC for bevacizumab in breast cancer
Question Results of ODAC (6 members)
Issue 1 Do the AVADO and RIBBON1 trials fail to verify the clinical benefit of Avastin for the breast cancer indication for which it was approved? Yes (agree for FDA): 6
No (agree for GNE): 0
 Yes: agree for FDA, No: agree for GNE
Issue 2A Does the available evidence on Avastin demonstrate that the drug has not been shown to be effective for the breast cancer indication for which it was approved? Yes (agree for FDA): 6
No (agree for GNE): 0
 Yes: agree for FDA,No: agree for GNE
Issue 2B Does the available evidence on Avastin demonstrate that the drug has not been shown to be safe for the breast cancer indication for which it was approved, in that Avastin has not been shown to present a clinical benefit that justifies the risks associated with use of the product for this indication? Yes (agree for FDA): 6
No (agree for GNE): 0
 Yes: agree for FDA,No: agree for GNE
Issue 3 If the Commissioner agrees with the grounds for withdrawal set out in issue 1, issue 2.A, or issue 2.B, should FDA nevertheless continue the approval of the breast cancer indica- tion while the sponsor designs and conducts additional studies intended to verify the drug’s clinical benefit? Yes (agree for GNE): 0
No (agree for FDA): 6
 Yes: agree for GNE,No: agree for FDA

ODAC, Oncology Drug Advisory Committee; AVADO, bevacizumab plus docetaxel in metastatic breast cancer; RIBBON, randomized, double-blind, placebo-controlled, phase III trial of chemotherapy with or without bevacizumab for first line treatment of HER2-negative locally recurrent or metastatic breast cancer; FDA, Food and Drug Administration; GNE, Genetec Co.

Table 8
Comparison of monotherapy with ipilimumab or GP100 peptide vaccine and the combination in patients with previously treated unresectable stage III or IV melanoma: Study MDX010-20 [38]
No. of patients No. of death Response rate (%) Median OS
(95% CI, mo)
Hazard ratio
(95% CI)
p-value
Ipilimumab+gp 100 403 306 5.7 10.0 (8.5-11.5)
0.68 (0.55-0.8) 0.00004
Placebo+gp 100 136 119 1.5 6.4 (5.5-8.7)
0.66 (0.51-0.87) 0.0026
Ipilimumab+placebo 137 100 10.9 10.1 (8.0-13.8)

OS, overall survival; CI, confidence interval.

Table 9
Comparison of ipilimumab (IPI) plus dacarbazine (DTIC) vs. DTIC alone as first line treatment in patients with unresectable stage III or IV melanoma [39]
IPI+ DTIC DTIC alone p-value
No. of patients 250 252
Response (CR+PR) (%) 38 (15.2) 26 (10.3)
Duration of response (mo) 9.3 8.1
Overall survival HR (95% CI) 0.72 (0.59-0.87) 0.0009
Median (mo) 11.2 9.1
Progression free survival HR (95% CI) 0.76 (0.63-0.93) 0.006
Median (mo) 2.8 2.6

CR, complete response; PR, partial response; HR, harzard ratio; CI, confidence interval.

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