北美协作组甲磺酸伊马替尼治疗晚期胃肠道间质瘤的III期试验中激酶基因型与临床结局的相关性:癌症与白血病B组及西南肿瘤协作组的CALGB 150105研究
Correlation of kinase genotype and clinical outcome in the North American Intergroup Phase III Trial of imatinib mesylate for treatment of advanced gastrointestinal stromal tumor: CALGB 150105 Study by Cancer and Leukemia Group B and Southwest Oncology Group.
作者信息
Heinrich Michael C, Owzar Kouros, Corless Christopher L, Hollis Donna, Borden Ernest C, Fletcher Christopher D M, Ryan Christopher W, von Mehren Margaret, Blanke Charles D, Rankin Cathryn, Benjamin Robert S, Bramwell Vivien H, Demetri George D, Bertagnolli Monica M, Fletcher Jonathan A
机构信息
Division of Hematology/Oncology, Department of Medicine and Cell and Developmental Biology, Portland Veterans Affairs Medical Center and Oregon Health and Science University Cancer Institute, Portland, OR 97239, USA.
出版信息
J Clin Oncol. 2008 Nov 20;26(33):5360-7. doi: 10.1200/JCO.2008.17.4284. Epub 2008 Oct 27.
PURPOSE
Imatinib mesylate is standard treatment for patients who have advanced gastrointestinal stromal tumor (GIST), but not all patients benefit equally. In previous studies, GIST genotype correlated with treatment outcome and optimal imatinib dosing.
PATIENTS AND METHODS
We examined the relationship between kinase genotype and treatment outcome for 428 patients enrolled on the North American phase III study SWOG S0033/CALGB 150105 and treated with either 400 mg or 800 mg daily doses of imatinib.
RESULTS
The presence of KIT exon 11-mutant genotype (n = 283) correlated with improved treatment outcome when compared with KIT exon 9-mutant (n = 32) and wild-type (WT; n = 67) genotypes for objective response (complete response [CR]/partial response [PR], 71.7% v 44.4% [P = .007]; and 44.6% [P = .0002], respectively); time to tumor progression (TTP; median 24.7 months v 16.7 and 12.8 months, respectively); and overall survival (OS; median 60.0 months v 38.4 and 49.0 months, respectively). The survival outcomes for patients with exon 9-mutant, exon 11-mutant or WT GIST were not affected by imatinib dose. However, there was evidence of improved response rates for patients with exon 9-mutant tumors treated with imatinib 800 mg versus 400 mg (CR/PR, 67% v 17%; P = .02). Patients who had CD117-negative GIST had similar TTP but inferior OS compared with patients who had CD117-positive disease, which suggests that patients who have CD117-negative GIST may benefit from imatinib treatment. In addition, we identified novel but rare mutations of the KIT extracellular domain (exons 8 and 9).
CONCLUSION
We confirmed the favorable impact of KIT exon 11 genotype when compared with KIT exon 9 and wild-type genotype for patients with advanced GIST who are treated with imatinib.
目的
甲磺酸伊马替尼是晚期胃肠道间质瘤(GIST)患者的标准治疗药物,但并非所有患者都能同等程度地获益。在既往研究中,GIST基因型与治疗结果及伊马替尼的最佳给药剂量相关。
患者与方法
我们在北美III期研究SWOG S0033/CALGB 150105中纳入了428例患者,这些患者接受每日400 mg或800 mg剂量的伊马替尼治疗,我们研究了激酶基因型与治疗结果之间的关系。
结果
与KIT外显子9突变型(n = 32)和野生型(WT;n = 67)基因型相比,KIT外显子11突变型基因型(n = 283)患者的治疗结果更佳,客观缓解率(完全缓解[CR]/部分缓解[PR])分别为71.7%、44.4%[P = 0.007]和44.6%[P = 0.0002];肿瘤进展时间(TTP)分别为中位数24.7个月、16.7个月和12.8个月;总生存期(OS)分别为中位数60.0个月、38.4个月和49.0个月。外显子9突变型、外显子11突变型或WT GIST患者的生存结果不受伊马替尼剂量的影响。然而,有证据表明,接受800 mg伊马替尼治疗的外显子9突变型肿瘤患者的缓解率高于接受400 mg治疗的患者(CR/PR分别为67%和17%;P = 0.02)。与CD117阳性疾病患者相比,CD117阴性GIST患者的TTP相似,但OS较差,这表明CD117阴性GIST患者可能从伊马替尼治疗中获益。此外,我们还发现了KIT细胞外结构域(外显子8和9)的新的但罕见的突变。
结论
我们证实,对于接受伊马替尼治疗的晚期GIST患者,与KIT外显子9和野生型基因型相比,KIT外显子11基因型具有有利影响。
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