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肿瘤标志物透明质酸和透明质酸酶1在前列腺癌中的基质和上皮表达

Stromal and epithelial expression of tumor markers hyaluronic acid and HYAL1 hyaluronidase in prostate cancer.

作者信息

Lokeshwar V B, Rubinowicz D, Schroeder G L, Forgacs E, Minna J D, Block N L, Nadji M, Lokeshwar B L

机构信息

Department of Urology, Cell Biology and Anatomy, and Pathology, University of Miami School of Medicine, Miami, Florida 33101, USA.

出版信息

J Biol Chem. 2001 Apr 13;276(15):11922-32. doi: 10.1074/jbc.M008432200. Epub 2001 Jan 19.

Abstract

Hyaluronic acid (HA), a glycosaminoglycan, regulates cell adhesion and migration. Hyaluronidase (HAase), an endoglycosidase, degrades HA into small angiogenic fragments. Using an enzyme-linked immunosorbent assay-like assay, we found increased HA levels (3-8-fold) in prostate cancer (CaP) tissues when compared with normal (NAP) and benign (BPH) tissues. The majority ( approximately 75-80%) of HA in prostate tissues was found to exist in the free form. Primary CaP fibroblast and epithelial cells secreted 3-8-fold more HA than respective NAP and BPH cultures. Only CaP epithelial cells and established CaP lines secreted HAase and the secretion increased with tumor grade and metastasis. The pH activity profile and optimum (4.2; range 4.0-4.3) of CaP HAase was identical to the HYAL1-type HAase present in human serum and urine. Full-length HYAL1 transcript and splice variants were detected in CaP cells by reverse transcriptase-polymerase chain reaction, cloning, and sequencing. Immunoblotting confirmed secretion of a approximately 60-kDa HYAL1-related protein by CaP cells. Immunohistochemistry showed minimal HA and HYAL1 staining in NAP and BPH tissues. However, a stromal and epithelial pattern of HA and HYAL1 expression was observed in CaP tissues. While high HA staining was observed in tumor-associated stroma, HYAL1 staining in tumor cells increased with tumor grade and metastasis. The gel-filtration column profiles of HA species in NAP, BPH, and CaP tissues were different. While the higher molecular mass and intermediate size HA was found in all tissues, the HA fragments were found only in CaP tissues. In particular, the high-grade CaP tissues, which showed both elevated HA and HYAL1 levels, contained angiogenic HA fragments. The stromal-epithelial HA and HYAL1 expression may promote angiogenesis in CaP and may serve as prognostic markers for CaP.

摘要

透明质酸(HA)是一种糖胺聚糖,可调节细胞黏附和迁移。透明质酸酶(HAase)是一种内切糖苷酶,可将HA降解为小的血管生成片段。通过一种类似酶联免疫吸附测定的检测方法,我们发现与正常(NAP)和良性(BPH)组织相比,前列腺癌(CaP)组织中的HA水平升高(3至8倍)。前列腺组织中大部分(约75 - 80%)的HA以游离形式存在。原发性CaP成纤维细胞和上皮细胞分泌的HA比相应的NAP和BPH培养物多3至8倍。只有CaP上皮细胞和已建立的CaP细胞系分泌HAase,且分泌量随肿瘤分级和转移而增加。CaP HAase的pH活性曲线和最佳值(4.2;范围4.0 - 4.3)与存在于人类血清和尿液中的HYAL1型HAase相同。通过逆转录聚合酶链反应、克隆和测序在CaP细胞中检测到全长HYAL1转录本和剪接变体。免疫印迹证实CaP细胞分泌一种约60 kDa的与HYAL1相关的蛋白质。免疫组织化学显示NAP和BPH组织中HA和HYAL1染色极少。然而,在CaP组织中观察到HA和HYAL1表达的基质和上皮模式。虽然在肿瘤相关基质中观察到高HA染色,但肿瘤细胞中的HYAL1染色随肿瘤分级和转移而增加。NAP、BPH和CaP组织中HA种类的凝胶过滤柱图谱不同。虽然在所有组织中都发现了较高分子量和中等大小的HA,但HA片段仅在CaP组织中发现。特别是,显示HA和HYAL1水平均升高的高级别CaP组织含有血管生成性HA片段。基质 - 上皮HA和HYAL1表达可能促进CaP中的血管生成,并可能作为CaP的预后标志物。

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