Rutkowski Piotr, Nowecki Zbigniew I, Debiec-Rychter Maria, Grzesiakowska Urszula, Michej Wanda, Woźniak Agnieszka, Siedlecki Janusz A, Limon Janusz, vel Dobosz Anna Jerzak, Kakol Michał, Osuch Czesław, Ruka Włodzimierz
Department of Soft Tissue/Bone Sarcoma and Melanoma, M. Sklodowska-Curie Memorial Cancer Center, Institute of Oncology, Warsaw, Poland.
J Cancer Res Clin Oncol. 2007 Sep;133(9):589-97. doi: 10.1007/s00432-007-0202-4. Epub 2007 Apr 26.
To analyze the outcomes of treatment and factors predicting effects of imatinib (IM) therapy in inoperable/metastatic gastrointestinal stromal tumors (GIST) CD117(+) patients.
We identified 232 patients in a prospectively collected Clinical GIST Registry with advanced inoperable/metastatic GIST treated with IM 400-800 mg daily (129 males and 103 females and median age 56 years). Median follow-up time was 26 months.
The estimated 3-year progression-free survival (PFS; calculated from the date of the start of IM) was 54% and median PFS was 40.5 months. The following factors significantly and negatively influenced PFS in univariate analysis: poor baseline World Health Organization (WHO) performance status > or = 2 (P < 0.00001), tumor genotype indicating other than KIT exon 11 isoform (P = 0.005), baseline high neutrophils count (P < 0.00001), age <45 years at the diagnosis (P = 0.04), mitotic index >10/50 high-power fields (HPF) (P = 0.001), GIST histological type other than spindle-cell (P = 0.03), baseline low albumin level (P = 0.0005), low baseline hemoglobin level (P < 0.00001), and primary overtly malignant tumors (unresectable and/or metastatic lesions at presentation) (P = 0.05). We identified four factors negatively affecting PFS, statistically significant (P < 0.05) in multivariate analysis: baseline poor WHO performance status > or = 2, high baseline neutrophils count (>5 x 10(9)/l), tumor genotype indicating the presence of non-exon 11 KIT mutant and mitotic index >10/50 HPF.
We confirmed that many advanced GIST patients benefit from IM therapy for a prolonged time, although resistance to therapy is observed. We identified four independent biological factors influencing the PFS during long-term IM therapy.
分析伊马替尼(IM)治疗不可切除/转移性胃肠道间质瘤(GIST)CD117(+)患者的治疗结果及预测疗效的因素。
我们在一项前瞻性收集的临床GIST注册研究中确定了232例晚期不可切除/转移性GIST患者,这些患者接受每日400 - 800 mg IM治疗(男性129例,女性103例,中位年龄56岁)。中位随访时间为26个月。
估计的3年无进展生存期(PFS;从IM开始日期计算)为54%,中位PFS为40.5个月。在单因素分析中,以下因素对PFS有显著负面影响:基线世界卫生组织(WHO)体能状态差≥2(P < 0.00001)、肿瘤基因型显示非KIT外显子11异构体(P = 0.005)、基线中性粒细胞计数高(P < 0.00001)、诊断时年龄<45岁(P = 0.04)、有丝分裂指数>10/50高倍视野(HPF)(P = 0.001)、GIST组织学类型不是梭形细胞型(P = 0.03)、基线白蛋白水平低(P = 0.0005)、基线血红蛋白水平低(P < 0.00001)以及原发性明显恶性肿瘤(初诊时不可切除和/或转移性病变)(P = 0.05)。我们确定了四个对PFS有负面影响的因素,在多因素分析中具有统计学意义(P < 0.05):基线WHO体能状态差≥2、基线中性粒细胞计数高(>5×10⁹/L)、肿瘤基因型显示存在非外显子11 KIT突变以及有丝分裂指数>10/50 HPF。
我们证实,尽管观察到对治疗有耐药性,但许多晚期GIST患者从IM治疗中获益时间延长。我们确定了四个影响长期IM治疗期间PFS的独立生物学因素。
