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Molecular cloning and characterization of a novel esophageal cancer related gene

机译:新型食管癌相关基因的分子克隆与鉴定

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We previously identified four novel cDNA fragments related to human esophageal cancer. One of the fragments was named esophageal cancer related gene 2 (ECRG2). We report here the molecular cloning, sequencing, and expression of the ECRG2 gene. The ECRG2 cDNA comprises a 258 bp nucleotide sequence which encodes for 85 amino acids with a predicted molecular weight of 9.2 kDa. Analysis of the protein sequence reveals the presence at the N terminus of a signal peptide followed by 56 amino acids with a significant degree of sequence similarity with the conserved Kazal domain which characterizes the serine protease inhibitor family. Pulse-chase experiments showed that ECRG2 protein was detected in both cell lysates and culture medium, indicating that the ECRG2 protein was extracellularly secreted after the post-translational cleavage. In vitro uPA/plasmin activity analysis showed the secreted ECRG2 protein inhibited the uPA/plasmin activity, indicating that ECRG2 may be a novel serine protease inhibitor. Northern blot analysis revealed the presence of the major band corresponding to a size of 569 kb throughout the fetal skin, thymus, esophagus, brain, lung, heart, stomach, liver, spleen, colon, kidney, testis, muscle, cholecyst tissues and adult esophageal mucosa, brain, thyroid tissue and mouth epithelia. However, ECRG2 gene was significantly down-regulated in primary esophageal cancer tissues. Taken together, these results indicate that ECRG2 is a novel member of the Kazal-type serine protease inhibitor family and may function as a tumor suppressor gene regulating the protease cascades during carcinogenesis and migration/invasion of esophageal cancer.
机译:我们先前确定了与人类食道癌相关的四个新的cDNA片段。这些片段之一被称为食道癌相关基因2(ECRG2)。我们在这里报告ECRG2基因的分子克隆,测序和表达。 ECRG2 cDNA包含一个258 bp的核苷酸序列,该序列编码85个氨基酸,预测分子量为9.2 kDa。对该蛋白质序列的分析揭示了在信号肽的N末端存在,随后是56个氨基酸,其与表征丝氨酸蛋白酶抑制剂家族的保守的Kazal结构域具有显着程度的序列相似性。脉冲追踪实验表明,在细胞裂解液和培养基中均检测到ECRG2蛋白,表明ECRG2蛋白在翻译后裂解后在细胞外分泌。体外uPA /纤溶酶活性分析表明,分泌的ECRG2蛋白抑制了uPA /纤溶酶活性,表明ECRG2可能是一种新型的丝氨酸蛋白酶抑制剂。 Northern印迹分析表明,在整个胎儿皮肤,胸腺,食道,脑,肺,心脏,胃,肝,脾,结肠,肾脏,睾丸,肌肉,胆囊组织和成人中,存在一条对应于569 kb大小的主要条带食道粘膜,脑,甲状腺组织和口腔上皮。但是,ECRG2基因在原发性食管癌组织中显着下调。综上所述,这些结果表明ECRG2是Kazal型丝氨酸蛋白酶抑制剂家族的新成员,并且可以在食管癌的致癌和迁移/侵袭过程中作为调节蛋白酶级联的肿瘤抑制基因起作用。

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