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人胰腺癌及相关转移病灶中的胰蛋白酶原和组织蛋白酶B

Pancreatic trypsinogen and cathepsin B in human pancreatic carcinomas and associated metastatic lesions.

作者信息

Ohta T, Terada T, Nagakawa T, Tajima H, Itoh H, Fonseca L, Miyazaki I

机构信息

Department of Surgery (II), School of Medicine, Kanazawa University, Japan.

出版信息

Br J Cancer. 1994 Jan;69(1):152-6. doi: 10.1038/bjc.1994.25.

Abstract

Expression of pancreatic trypsinogen and cathepsin B in 23 surgically resected pancreatic ductal adenocarcinomas was evaluated immunohistochemically, using a monoclonal antibody against human pancreatic trypsinogen and a polyclonal antibody against human cathepsin B. Fifteen of 20 invasive tubular adenocarcinomas (75%) expressed pancreatic trypsinogen in a coarse granular pattern located in the supranuclear cytoplasm of the carcinoma cells. In addition, metastatic lesions, including those in peripancreatic lymph nodes and neural plexuses, expressed pancreatic trypsinogen. In contrast, three intraductal (non-invasive) papillary adenocarcinomas did not express pancreatic trypsinogen. Cathepsin B expression was recognised in 14 of 20 invasive tubular adenocarcinomas (70%) in a fine granular pattern located diffusely in the cytoplasm of the carcinoma cells, while none of the three intraductal papillary adenocarcinomas had detectable cathepsin B. These findings suggest that pancreatic invasive ductal adenocarcinomas express pancreatic trypsinogen and cathepsin B immunoreactive peptides, raising the possibility that pancreatic trypsinogen and cathepsin B may act independently of each other in the process of carcinoma invasion and metastasis, like other different classes of proteases involved in the proteolytic modification of the matrix barrier.

摘要

采用抗人胰蛋白酶原单克隆抗体和抗人组织蛋白酶B多克隆抗体,通过免疫组织化学方法评估了23例手术切除的胰腺导管腺癌中胰蛋白酶原和组织蛋白酶B的表达情况。20例浸润性管状腺癌中有15例(75%)以位于癌细胞核上细胞质中的粗颗粒模式表达胰蛋白酶原。此外,转移灶,包括胰周淋巴结和神经丛中的转移灶,也表达胰蛋白酶原。相比之下,3例导管内(非浸润性)乳头状腺癌不表达胰蛋白酶原。20例浸润性管状腺癌中有14例(70%)以弥漫分布于癌细胞细胞质中的细颗粒模式识别出组织蛋白酶B的表达,而3例导管内乳头状腺癌均未检测到组织蛋白酶B。这些发现表明,胰腺浸润性导管腺癌表达胰蛋白酶原和组织蛋白酶B免疫反应性肽,这增加了胰蛋白酶原和组织蛋白酶B在癌侵袭和转移过程中可能像其他参与基质屏障蛋白水解修饰的不同类蛋白酶一样相互独立发挥作用的可能性。

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