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组织蛋白酶B在人前列腺肿瘤中的免疫组织化学定位

Immunohistochemical localization of cathepsin B in neoplastic human prostate.

作者信息

Sinha A A, Wilson M J, Gleason D F, Reddy P K, Sameni M, Sloane B F

机构信息

Research Service, Veterans Affairs Medical Center, Minneapolis, MN 55417, USA.

出版信息

Prostate. 1995 Apr;26(4):171-8. doi: 10.1002/pros.2990260402.

Abstract

Cathepsin B (CB) has been shown to degrade extracellular matrix (ECM) proteins, and has been reported to be involved in invasion and metastasis of several types of solid organ tumors in human and animals, but CB has not been studied in human prostate cancer (CAP). Our objective was to determine the CB protein immunostaining pattern in CAP and to correlate the immunostaining with the degree of malignancy as reflected in the Gleason grading system. We used two types of CB antibodies (namely, monospecific, polyclonal antibodies to human liver CB prepared in rabbits, and polyclonal antibody produced in sheep) to establish CB localization patterns in neoplastic prostate. Our analysis showed a heterogeneous CB immunostaining pattern in the neoplastic human prostate. CB immunostaining occurred in many, but not all, of the neoplastic columnar/cuboidal cells of acini and isolated cells, i.e., in small ragged glands and clusters (groups) of invasive cells in the prostatic stroma. We have shown that, in general, there was a positive correlation of the intensity of CB immunostaining with the Gleason histologic score (or Gleason grade sum) tumors, i.e., from the lowest scores through score 8, but many of the tumors with scores 9 and 10 showed little CB immunostaining. Our study indicated that the increased CB immunostaining in the Gleason grade sum 5-8 tumors may be associated with increased degradation of ECM, but not in 9 and 10 despite the fact that the latter tumors are more malignant clinically. In well-differentiated tumors, fewer CB immunostaining cells were present than the moderately-differentiated tumors. In other words, most of the stromal invasion of the prostatic ECM occurred in tumors of Gleason grade sums 5-8. We suggest that CB immunostaining might be a useful method to assess stromal invasion of prostatic carcinoma, especially in the higher grade tumors.

摘要

组织蛋白酶B(CB)已被证明可降解细胞外基质(ECM)蛋白,并且据报道它参与人类和动物多种实体器官肿瘤的侵袭和转移,但尚未在人类前列腺癌(CAP)中进行研究。我们的目的是确定CAP中CB蛋白的免疫染色模式,并将免疫染色与Gleason分级系统所反映的恶性程度相关联。我们使用两种类型的CB抗体(即兔制备的针对人肝脏CB的单特异性多克隆抗体,以及绵羊产生的多克隆抗体)来确定肿瘤性前列腺中CB的定位模式。我们的分析显示,在肿瘤性人类前列腺中存在异质性的CB免疫染色模式。CB免疫染色出现在许多但并非所有的腺泡肿瘤性柱状/立方体细胞和孤立细胞中,即在前列腺基质中的小而不规则的腺体以及侵袭性细胞簇(组)中。我们已经表明,一般来说,CB免疫染色强度与肿瘤的Gleason组织学评分(或Gleason分级总和)呈正相关,即从最低评分到8分,但许多评分9分和10分的肿瘤显示很少的CB免疫染色。我们的研究表明,Gleason分级总和为5 - 8分的肿瘤中CB免疫染色增加可能与ECM降解增加有关,但9分和10分的肿瘤并非如此,尽管后一种肿瘤在临床上恶性程度更高。在高分化肿瘤中,CB免疫染色细胞比中分化肿瘤少。换句话说,前列腺ECM的大多数基质侵袭发生在Gleason分级总和为5 - 8分的肿瘤中。我们建议,CB免疫染色可能是评估前列腺癌基质侵袭的一种有用方法,特别是在高分级肿瘤中。

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