Gonçalves Anthony, Esteyries Séverine, Taylor-Smedra Brynn, Lagarde Arnaud, Ayadi Mounay, Monges Geneviève, Bertucci François, Esterni Benjamin, Delpero Jean-Robert, Turrini Olivier, Lelong Bernard, Viens Patrice, Borg Jean-Paul, Birnbaum Daniel, Olschwang Sylviane, Viret Frédéric
Department of Medical Oncology, Institut Paoli-Calmettes, Marseille, France.
BMC Cancer. 2008 Jun 10;8:169. doi: 10.1186/1471-2407-8-169.
Cetuximab, a monoclonal antibody targeting Epidermal Growth Factor Receptor (EGFR), is currently used in metastatic colorectal cancer (mCRC), but predictive factors for therapeutic response are lacking. Mutational status of KRAS and EGFR, and EGFR copy number are potential determinants of cetuximab activity.
We analyzed tumor tissues from 32 EGFR-positive mCRC patients receiving cetuximab/irinotecan combination and evaluable for treatment response. EGFR copy number was quantified by fluorescence in situ hybridization (FISH). KRAS exon 1 and EGFR exons coding for extracellular regions were sequenced.
Nine patients experienced an objective response (partial response) and 23 were considered as nonresponders (12 with stable disease and 11 with progressive disease). There was no EGFR amplification found, but high polysomy was noted in 2 patients, both of which were cetuximab responders. No EGFR mutations were found but a variant of exon 13 (R521K) was observed in 12 patients, 11 of which achieved objective response or stable disease. Progression-free and overall survivals were significantly better in patients with this EGFR exon 13 variant. KRAS mutations were found in 14 cases. While there was a trend for an increased KRAS mutation frequency in nonresponder patients (12 mutations out of 23, 52%) as compared to responder patients (2 out of 9, 22%), authentic tumor response or long-term disease stabilization was found in KRAS mutated patients.
This preliminary study suggests that: an increase in EGFR copy number may be associated with cetuximab response but is a rare event in CRC, KRAS mutations are associated with low response rate but do not preclude any cetuximab-based combination efficacy and EGFR exon 13 variant (R521K) may predict for cetuximab benefit.
西妥昔单抗是一种靶向表皮生长因子受体(EGFR)的单克隆抗体,目前用于转移性结直肠癌(mCRC),但缺乏治疗反应的预测因素。KRAS和EGFR的突变状态以及EGFR拷贝数是西妥昔单抗活性的潜在决定因素。
我们分析了32例接受西妥昔单抗/伊立替康联合治疗且可评估治疗反应的EGFR阳性mCRC患者的肿瘤组织。通过荧光原位杂交(FISH)对EGFR拷贝数进行定量。对KRAS外显子1和编码细胞外区域的EGFR外显子进行测序。
9例患者出现客观反应(部分缓解),23例被视为无反应者(12例病情稳定,11例病情进展)。未发现EGFR扩增,但2例患者出现高多体性,这2例均为西妥昔单抗反应者。未发现EGFR突变,但在12例患者中观察到外显子13的一个变体(R521K),其中11例实现了客观反应或病情稳定。具有这种EGFR外显子13变体的患者的无进展生存期和总生存期明显更好。14例患者发现KRAS突变。与反应者患者(9例中的2例,22%)相比,无反应者患者(23例中的12例突变,52%)的KRAS突变频率有增加趋势,但在KRAS突变患者中发现了真实的肿瘤反应或长期疾病稳定。
这项初步研究表明:EGFR拷贝数增加可能与西妥昔单抗反应相关,但在结直肠癌中是罕见事件;KRAS突变与低反应率相关,但不排除任何基于西妥昔单抗的联合疗效;EGFR外显子13变体(R521K)可能预测西妥昔单抗治疗有益。
