中华外科杂志
中華外科雜誌
중화외과잡지
CHINESE JOURNAL OF SURGERY
2009年
11期
857-862
,共6页
赵文毅%曹晖%张云%沈志勇%吴志勇
趙文毅%曹暉%張雲%瀋誌勇%吳誌勇
조문의%조휘%장운%침지용%오지용
胃肠道间质肿瘤%预后%c-kit基因%伊马替尼
胃腸道間質腫瘤%預後%c-kit基因%伊馬替尼
위장도간질종류%예후%c-kit기인%이마체니
Gastrointestinal stromal tumors%Prognosis%c-kit gene%Imatinih
目的 探讨c-kit基因突变对胃肠道间质瘤(GIST)预后的影响.方法 通过电子检索PubMed、MedLine数据库,对1999年1月至2008年8月有关c-kit基因突变对GIST预后影响相关病例对照研究资料,用RevMan 5.0.15软件进行荟萃分析.结果 共纳入文献16篇,共计患者1751例.其中与细胞病理学相关统计显示c-kit基因野生型与突变型在有丝分裂计数>5/50 HPF(高倍视野)的病例发生率上差异无统计学意义(P=0.710);与术后复发转移发生率相关统计显示,c-kit基因突变型术后复发转移的发生率显著高于野生型者(P=0.010);与伊马替尼疗效相关统计显示,c-kit基因突变型患者伊马替尼治疗缓解率显著高于野生型(P=0.009),而伊马替尼耐药率较低(P=0.000).亚组分析发现,外显子11突变型的患者伊马替尼治疗缓解率显著高于野生型和外显子9突变型者(P均<0.05),而伊马替尼耐药率较低(P均<0.05).c-kit基因二次突变与伊马替尼获得性耐药相关研究发现,二次突变区域集中在外显子13、14和17,部分为混合型突变.结论 c-kit基因突变与GIST术后复发转移的发生有着密切关系,c-kit基因突变可能会影响伊马替尼的疗效,而二次突变的发生可能是GIST产生耐药的主要原因之一.
目的 探討c-kit基因突變對胃腸道間質瘤(GIST)預後的影響.方法 通過電子檢索PubMed、MedLine數據庫,對1999年1月至2008年8月有關c-kit基因突變對GIST預後影響相關病例對照研究資料,用RevMan 5.0.15軟件進行薈萃分析.結果 共納入文獻16篇,共計患者1751例.其中與細胞病理學相關統計顯示c-kit基因野生型與突變型在有絲分裂計數>5/50 HPF(高倍視野)的病例髮生率上差異無統計學意義(P=0.710);與術後複髮轉移髮生率相關統計顯示,c-kit基因突變型術後複髮轉移的髮生率顯著高于野生型者(P=0.010);與伊馬替尼療效相關統計顯示,c-kit基因突變型患者伊馬替尼治療緩解率顯著高于野生型(P=0.009),而伊馬替尼耐藥率較低(P=0.000).亞組分析髮現,外顯子11突變型的患者伊馬替尼治療緩解率顯著高于野生型和外顯子9突變型者(P均<0.05),而伊馬替尼耐藥率較低(P均<0.05).c-kit基因二次突變與伊馬替尼穫得性耐藥相關研究髮現,二次突變區域集中在外顯子13、14和17,部分為混閤型突變.結論 c-kit基因突變與GIST術後複髮轉移的髮生有著密切關繫,c-kit基因突變可能會影響伊馬替尼的療效,而二次突變的髮生可能是GIST產生耐藥的主要原因之一.
목적 탐토c-kit기인돌변대위장도간질류(GIST)예후적영향.방법 통과전자검색PubMed、MedLine수거고,대1999년1월지2008년8월유관c-kit기인돌변대GIST예후영향상관병례대조연구자료,용RevMan 5.0.15연건진행회췌분석.결과 공납입문헌16편,공계환자1751례.기중여세포병이학상관통계현시c-kit기인야생형여돌변형재유사분렬계수>5/50 HPF(고배시야)적병례발생솔상차이무통계학의의(P=0.710);여술후복발전이발생솔상관통계현시,c-kit기인돌변형술후복발전이적발생솔현저고우야생형자(P=0.010);여이마체니료효상관통계현시,c-kit기인돌변형환자이마체니치료완해솔현저고우야생형(P=0.009),이이마체니내약솔교저(P=0.000).아조분석발현,외현자11돌변형적환자이마체니치료완해솔현저고우야생형화외현자9돌변형자(P균<0.05),이이마체니내약솔교저(P균<0.05).c-kit기인이차돌변여이마체니획득성내약상관연구발현,이차돌변구역집중재외현자13、14화17,부분위혼합형돌변.결론 c-kit기인돌변여GIST술후복발전이적발생유착밀절관계,c-kit기인돌변가능회영향이마체니적료효,이이차돌변적발생가능시GIST산생내약적주요원인지일.
Objective To investigate the effect of c-kit mutation on the prognosis of gastrointestinal stremal tumors. Methods A search of studies in PubMed and MedLine (from 1999 to 2008) was performed to assess the effect of c-kit mutation on the prognosis of gastrointestinal strernal tumors. The articles were retrieved with the entries of "gastrointestinal stromal tumors", "imatinib" ,"c-kit" and "mutation". A recta-analysis was performed to assess the data included. Results A total of 15 articles were collected in this analysis. No significant differences was found in incidence of mitoses ( >5/50 HPF) between the patients with wild type c-kit (wild type group) and the ones with mutated c-kit (mutation group) (P=0.710); tumor recurrence and metastasis rate after surgery was significant higher in the mutation group than that in wild type group(P=0.010) ; as for imatinib response with different c-kit mutation types, the results showed the incidence of clinical response(complete response + partial response) was significantly higher in mutation group than that in wild type group(P =0. 009) ,but the imatinib resistance rate was lower in mutation group (P=0.000) ; three studies prodded data for imatinib resistance with c-kit second mutations, the results showed the second mutations mainly focus on exon 13, 14, 17. Conclusions C-kit mutation is related closely with the incidence of recurrence and metastasis in GIST after surgery. The mutations of c-kit influences the therapeutic effects of imatinib.
