中华皮肤科杂志
中華皮膚科雜誌
중화피부과잡지
Chinese Journal of Dermatology
2013年
8期
565-569
,共5页
黄莹雪%周璐%张韡%邵雪宝%李阿梅%徐秀莲%孙建方
黃瑩雪%週璐%張韡%邵雪寶%李阿梅%徐秀蓮%孫建方
황형설%주로%장위%소설보%리아매%서수련%손건방
黑色素瘤%金属蛋白酶类组织抑制剂%基质金属蛋白酶类
黑色素瘤%金屬蛋白酶類組織抑製劑%基質金屬蛋白酶類
흑색소류%금속단백매류조직억제제%기질금속단백매류
Melanoma%Tissue inhibitor of metalloproteinases%Matrix metalloproteinases
目的 探讨基质金属蛋白酶抑制剂4(TIMP-4)在皮肤恶性黑素瘤(CMM)中的表达及其与肿瘤增殖、侵袭和转移的相关性.方法 应用蛋白免疫印迹方法分析5例CMM和瘤旁组织及3例色素痣组织中TIMP-4蛋白表达差异.应用免疫组化法检测TIMP-4在43例CMM和51例色素痣组织中的表达,并分析其与临床病理特征、Ki-67、基质金属蛋白酶2(MMP-2)、血管内皮细胞生长因子(VEGF)及黑素瘤表面标志物CD63表达的相关性.免疫组化法检测Ki-67、MMP-2、VEGF和CD63表达.结果 Western印迹结果提示,5例CMM组织中4例TIMP-4表达高于瘤旁组织和3例色素痣组织.免疫组化分析结果,TIMP-4在43例CMM和51例色素痣中分别有37例和10例阳性,阳性率分别为86.04%和19.6%,两组差异有统计学意义(x2=31.55,P< 0.05).TIMP-4表达水平与CMM的进展呈正相关(rs=0.309,P< 0.05),随着肿瘤从原位到侵袭性再发展到转移性,TIMP-4表达水平呈升高趋势.CMM中TIMP-4表达与临床分期、肿瘤厚度、Clark分级、溃疡与否等预后变量无显著相关性,与Ki-67亦无显著相关,但TIMP-4表达与VEGF表达呈正相关(rs=0.345,P< 0.05);CMM中MMP-2阳性组TIMP-4的表达明显高于MMP-2阴性组(P<0.01);此外,TIMP-4表达与CD63表达呈正相关(rs=0.555,P< 0.01).结论 TIMP-4在CMM中呈高表达,可能参与CMM的发生及发展,尤其与其转移及血管生成密切相关.
目的 探討基質金屬蛋白酶抑製劑4(TIMP-4)在皮膚噁性黑素瘤(CMM)中的錶達及其與腫瘤增殖、侵襲和轉移的相關性.方法 應用蛋白免疫印跡方法分析5例CMM和瘤徬組織及3例色素痣組織中TIMP-4蛋白錶達差異.應用免疫組化法檢測TIMP-4在43例CMM和51例色素痣組織中的錶達,併分析其與臨床病理特徵、Ki-67、基質金屬蛋白酶2(MMP-2)、血管內皮細胞生長因子(VEGF)及黑素瘤錶麵標誌物CD63錶達的相關性.免疫組化法檢測Ki-67、MMP-2、VEGF和CD63錶達.結果 Western印跡結果提示,5例CMM組織中4例TIMP-4錶達高于瘤徬組織和3例色素痣組織.免疫組化分析結果,TIMP-4在43例CMM和51例色素痣中分彆有37例和10例暘性,暘性率分彆為86.04%和19.6%,兩組差異有統計學意義(x2=31.55,P< 0.05).TIMP-4錶達水平與CMM的進展呈正相關(rs=0.309,P< 0.05),隨著腫瘤從原位到侵襲性再髮展到轉移性,TIMP-4錶達水平呈升高趨勢.CMM中TIMP-4錶達與臨床分期、腫瘤厚度、Clark分級、潰瘍與否等預後變量無顯著相關性,與Ki-67亦無顯著相關,但TIMP-4錶達與VEGF錶達呈正相關(rs=0.345,P< 0.05);CMM中MMP-2暘性組TIMP-4的錶達明顯高于MMP-2陰性組(P<0.01);此外,TIMP-4錶達與CD63錶達呈正相關(rs=0.555,P< 0.01).結論 TIMP-4在CMM中呈高錶達,可能參與CMM的髮生及髮展,尤其與其轉移及血管生成密切相關.
목적 탐토기질금속단백매억제제4(TIMP-4)재피부악성흑소류(CMM)중적표체급기여종류증식、침습화전이적상관성.방법 응용단백면역인적방법분석5례CMM화류방조직급3례색소지조직중TIMP-4단백표체차이.응용면역조화법검측TIMP-4재43례CMM화51례색소지조직중적표체,병분석기여림상병리특정、Ki-67、기질금속단백매2(MMP-2)、혈관내피세포생장인자(VEGF)급흑소류표면표지물CD63표체적상관성.면역조화법검측Ki-67、MMP-2、VEGF화CD63표체.결과 Western인적결과제시,5례CMM조직중4례TIMP-4표체고우류방조직화3례색소지조직.면역조화분석결과,TIMP-4재43례CMM화51례색소지중분별유37례화10례양성,양성솔분별위86.04%화19.6%,량조차이유통계학의의(x2=31.55,P< 0.05).TIMP-4표체수평여CMM적진전정정상관(rs=0.309,P< 0.05),수착종류종원위도침습성재발전도전이성,TIMP-4표체수평정승고추세.CMM중TIMP-4표체여림상분기、종류후도、Clark분급、궤양여부등예후변량무현저상관성,여Ki-67역무현저상관,단TIMP-4표체여VEGF표체정정상관(rs=0.345,P< 0.05);CMM중MMP-2양성조TIMP-4적표체명현고우MMP-2음성조(P<0.01);차외,TIMP-4표체여CD63표체정정상관(rs=0.555,P< 0.01).결론 TIMP-4재CMM중정고표체,가능삼여CMM적발생급발전,우기여기전이급혈관생성밀절상관.
Objective To detect the expression of tissue inhibitor of metalloproteinase-4 (TIMP-4) in cutaneous malignant melanoma (CMM) tissue and to assess its relationship with melanoma proliferation,invasion and metastasis.Methods Western blot was conducted to measure the protein expression of TIMP-4 in five fresh lesional and paratumoral tissue specimens of CMM and three fresh tissue specimens of nevi.Immunohistochemistry was carried out to quantify the expression of TIMP-4,Ki-67,matrix metalloproteinase-2 (MMP-2),vascular endothelial growth factor (VEGF) and CD63 in paraffin-embedded tissue samples from 43 cases of CMM and 51 cases of nevi.The degree of malignancy of melanoma was evaluated in these lesions.Results Western blot analysis showed that the expression of TIMP-4 was significantly higher in 4 of 5 CMM tissue specimens than in corresponding paratumoral tissue specimens and nevus tissue specimens.Immunohistochemistry revealed that the expression rate of TIMP-4 was 86.04% (37/43) in melanoma tissue,compared to 19.6% (10/51) in nevus tissue (x2 =31.55,P < 0.05).The expression of TIMP-4 increased sequentially from in situ melanoma to invasive and metastatic melanoma (rs =0.309,P < 0.05).As far as CMM was concerned,the TIMP-4 expression was uncorrelated with any of the known prognostic variables including clinical stage,Clark level,Breslow depth,presence of ulcer,and Ki-67 expression (all P > 0.05),but positively correlated with the expressions of VEGF (rs =0.345,P < 0.05) and CD63 (rs =0.555,P < 0.01).The median expression level of TIMP-4 was significantly higher in MMP-2-positive than in MMP-2-negative melanoma tissue samples (3 vs.0,P < 0.01).Conclusions TIMP-4 protein is highly expressed in CMM tissue,which may be closely associated with the initiation and progression of CMM,especially with the metastasis of and angiogenesis in CMM.