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干细胞因子及其受体c-kit蛋白在正常睾丸组织和恶性生殖细胞肿瘤中的表达

Expression of stem-cell factor and its receptor c-kit protein in normal testicular tissue and malignant germ-cell tumours.

作者信息

Bokemeyer C, Kuczyk M A, Dunn T, Serth J, Hartmann K, Jonasson J, Pietsch T, Jonas U, Schmoll H J

机构信息

Department of Haematology/Oncology, Hannover University Medical School, Hannover, Germany.

出版信息

J Cancer Res Clin Oncol. 1996;122(5):301-6. doi: 10.1007/BF01261407.

Abstract

The proto-oncogene c-kit and its ligand stem-cell factor (SCF) may play an important role in the development of normal and malignant testicular tissue. This study investigates the presence of SCF and c-kit protein in 32 orchiectomy specimens of patients with testicular cancer, in 5 specimens of normal testicular tissue and in three established non-seminomatous germ-cell cancer cell lines (H12.1, H32, 577ML) by an immunohistochemical approach. Out of 9 testicular cancer specimens classified as pure seminomas, 7 (78%) showed a strong immunohistochemical reaction for both SCF and c-kit protein on the surface of the tumour cells. Fourteen non-seminomatous germ-cell tumours composed of embryonal carcinoma were completely negative for both SCF and c-kit proteins and only faint positivity was found in 6 tumours (26%). Differentiated teratomatous structures within the specimens on non-seminomatous tumours showed a strong immunohistochemical reaction for SCF and c-kit protein in 8 of 11 (73%) cases. All three testicular cancer cell lines showed only faint staining reactions for c-kit protein and none for SCF. No secretion of SCF by the three lines in vitro was detected. The addition of high concentrations of SCF (100 ng/ml) to the testicular cancer cell lines in culture conditions without fetal calf serum resulted in a 1.4 to 3-fold growth stimulation compared to cell growth in serum-free medium alone. This effect was not detectable when the cells were cultured in serum-containing media. In the normal testicular tissue the germ-cells displayed a strong immunohistochemical reaction for c-kit protein while SCF positivity was found at the tubular membrane and on the surface of Sertoli cells. The SCF/c-kit system may possess a regulatory function in normal testicular tissue by possibly providing the microenvironment necessary for spermatogenesis. With the development of testicular cancer, this regulatory system seems to be lost, particularly in non-seminomatous germ-cell tumours. A growth-stimulatory effect of high concentrations of SCF on non-seminomatous testicular cancer cell lines can be detected only in culture conditions with serum-free media. The effects achievable by the combination of SCF with other growth factors need to be further studied, as well as the role of the c-kit/SCF regulatory system for normal spermatogenesis and its possible implications for the understanding and treatment of male infertility.

摘要

原癌基因c-kit及其配体干细胞因子(SCF)可能在正常和恶性睾丸组织的发育中起重要作用。本研究采用免疫组织化学方法,检测了32例睾丸癌患者的睾丸切除标本、5例正常睾丸组织标本以及三种已建立的非精原性生殖细胞癌细胞系(H12.1、H32、577ML)中SCF和c-kit蛋白的表达情况。在9例被归类为纯精原细胞瘤的睾丸癌标本中,7例(78%)肿瘤细胞表面的SCF和c-kit蛋白免疫组织化学反应强烈。14例由胚胎癌组成的非精原性生殖细胞肿瘤的SCF和c-kit蛋白均呈完全阴性,仅6例肿瘤(26%)呈弱阳性。非精原性肿瘤标本中的分化畸胎瘤结构在11例中有8例(73%)对SCF和c-kit蛋白呈强烈免疫组织化学反应。所有三种睾丸癌细胞系对c-kit蛋白仅呈弱阳性反应,对SCF均无反应。未检测到这三种细胞系在体外分泌SCF。在无胎牛血清的培养条件下,向睾丸癌细胞系中添加高浓度的SCF(100 ng/ml),与仅在无血清培养基中培养的细胞相比,细胞生长受到1.4至3倍的刺激。当细胞在含血清的培养基中培养时,未检测到这种效应。在正常睾丸组织中,生殖细胞对c-kit蛋白呈强烈免疫组织化学反应,而在管状膜和支持细胞表面发现SCF呈阳性。SCF/c-kit系统可能通过提供精子发生所需的微环境,在正常睾丸组织中发挥调节功能。随着睾丸癌的发展,这种调节系统似乎丧失,尤其是在非精原性生殖细胞肿瘤中。仅在无血清培养基的培养条件下,才能检测到高浓度SCF对非精原性睾丸癌细胞系的生长刺激作用。SCF与其他生长因子联合使用所能达到的效果,以及c-kit/SCF调节系统对正常精子发生的作用及其对男性不育症理解和治疗的可能影响有待进一步研究。

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