Nystrom Scott J, Hornberger John C, Varadhachary Gauri R, Hornberger Richard J, Gutierrez Hialy R, Henner David W, Becker Shawn H, Amin Mahul B, Walker Michael G
Department of Medicine, Tufts Medical Center, Boston, MA, USA.
Oncotarget. 2012 Jun;3(6):620-8. doi: 10.18632/oncotarget.521.
The primary tissue-site origin in over 4% of cancers remains uncertain despite thorough clinicopathological evaluation. This study assessed the effect of a Food and Drug Administration-cleared 2,000- gene-expression-profiling (GEP) test on primary tissue-site working diagnoses and management for metastatic and poorly differentiated cancers.
Clinical information was collected from physicians ordering the GEP test for patients with difficult to diagnose cancers. Endpoints included diagnostic procedures, physicians' working diagnoses and treatment recommendations before and after GEP result availability, and physician reports of the test's usefulness for clinical decision making. Patient date of death was obtained, with a minimum of one year follow-up from date of biopsy.
Sixty-five physicians participated in the study (n=107 patients). Before GEP, patients underwent 3.2 investigations on average (e.g., radiology, endoscopy). Ten immunohistochemistry tests were used per biopsy (SD 5.2). After GEP testing, physicians changed the primary working diagnosis for 50% of patients (95% CI: 43%,58%) and management for 65% of patients (95% CI: 58%,73%). With GEP results, the recommendation for guideline-consistent chemotherapy increased from 42% to 65% of patients, and the recommendation for non-guideline-consistent regimens declined from 28% to 13%. At last follow-up, 69 patients had died, and median survival was 14.0 months (95% CI: 10.2,18.6). Thirty-three percent of patients were alive at 2 years.
In patients with difficult-to-diagnose cancers, GEP changed the working diagnosis and management for the majority of patients. Patients for whom the GEP test was ordered had longer median survival than that historically reported for patients enrolled in treatment trials for cancer of unknown primary.
尽管进行了全面的临床病理评估,但超过4%的癌症的原发组织部位来源仍不明确。本研究评估了一项经美国食品药品监督管理局批准的2000基因表达谱(GEP)检测对转移性和低分化癌症的原发组织部位工作诊断及管理的影响。
从为难以诊断的癌症患者订购GEP检测的医生处收集临床信息。终点指标包括诊断程序、GEP结果可得前后医生的工作诊断和治疗建议,以及医生关于该检测对临床决策有用性的报告。获取患者的死亡日期,自活检日期起至少随访一年。
65名医生参与了该研究(n = 107例患者)。在进行GEP检测之前,患者平均接受了3.2项检查(如放射学、内镜检查)。每次活检使用10次免疫组化检测(标准差5.2)。在进行GEP检测后,医生改变了50%患者的主要工作诊断(95%置信区间:43%,58%)以及65%患者的管理方案(95%置信区间:58%,73%)。根据GEP结果,符合指南的化疗建议从42%的患者增加到65%,不符合指南方案的建议从28%降至13%。在最后一次随访时,69例患者已死亡,中位生存期为14.0个月(95%置信区间:10.2,18.6)。33%的患者在2年时仍存活。
在难以诊断的癌症患者中,GEP改变了大多数患者的工作诊断和管理方案。接受GEP检测的患者的中位生存期长于历史上报道的不明原发癌治疗试验入组患者的生存期。
