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犬乳腺肿瘤中p53基因产物的过表达。

Overexpression of the p53 gene product in canine mammary tumors.

作者信息

Haga S, Nakayama M, Tatsumi K, Maeda M, Imai S, Umesako S, Yamamoto H, Hilgers J, Sarkar N H

机构信息

The Second Department of Anatomy, Nara Medical University, Kashihara-City, Nara 634-8521, Japan.

出版信息

Oncol Rep. 2001 Nov-Dec;8(6):1215-9. doi: 10.3892/or.8.6.1215.

Abstract

p53, a tumor suppressor gene, is a target of genetic alternations in many human and animal cancers. Compared to normal tissues, cancer tissues overexpress mutant p53 protein thus allowing their detection by a number of immunochemical procedures. To what extent the expression of mutant p53 correlates with dog mammary tumorigenesis has not been fully studied. In the present study, 20 spontaneously arising canine mammary tumors were examined for overexpression of mutant p53. Two different monoclonal antibodies, BP53-12 and PAb122, which recognize different epitopes of the p53 product, were used. The canine tumors in the present study exhibited five different histological types: i) osteosarcoma (n=7); ii) carcinosarcoma (n=4); iii) solid carcinoma (n=5); iv) complex carcinoma (n=3); and v) tubulopapillar carcinoma (n=1). The positive ratios against BP53-12 and PAb122 antibodies were 50% (10/20) and 60% (12/20) respectively. Among these positive samples, 35% (7/20) reacted to both antibodies. Finally, 15 out of 20 tumors showed positivity against one of the monoclonal antibodies. Mostly, as in human mammary tumor cells, BP53-12 staining was observed in the nuclei of tumor cells. PAb122 staining, however, was confined to cytoplasm of osteosarcoma or carcinosarcoma cells. To confirm the location of the staining, immunoelectron microscopy was done. The results showed that the cytoplasm of cartilage cells in the sarcomas had positive staining. These results indicate that anti-p53 antibodies BP53-12 and PAb122, generated against human p53 are cross reacting with the same molecule in canine cells and that the role of p53 in tumorigenesis is not only confined to tumors in human. Our finding suggests that a combination of p53 monoclonal antibodies should be used to screen, not only canine mammary tumors but also human mammary tumors, to obtain a better tumor prognosis.

摘要

p53是一种肿瘤抑制基因,是许多人类和动物癌症中基因改变的靶点。与正常组织相比,癌组织中突变型p53蛋白过度表达,因此可以通过多种免疫化学方法检测到。突变型p53的表达与犬乳腺肿瘤发生的关联程度尚未得到充分研究。在本研究中,对20例自发产生的犬乳腺肿瘤进行了突变型p53过度表达检测。使用了两种识别p53产物不同表位的不同单克隆抗体,即BP53 - 12和PAb122。本研究中的犬肿瘤表现出五种不同的组织学类型:i)骨肉瘤(n = 7);ii)癌肉瘤(n = 4);iii)实体癌(n = 5);iv)复合癌(n = 3);v)管状乳头状癌(n = 1)。针对BP53 - 12和PAb122抗体的阳性率分别为50%(10/20)和60%(12/20)。在这些阳性样本中,35%(7/20)对两种抗体均有反应。最后,20个肿瘤中有15个对其中一种单克隆抗体呈阳性。与人类乳腺肿瘤细胞一样,大多数情况下,BP53 - 12染色见于肿瘤细胞核。然而,PAb122染色局限于骨肉瘤或癌肉瘤细胞的细胞质。为了确认染色位置,进行了免疫电子显微镜检查。结果显示肉瘤中软骨细胞的细胞质有阳性染色。这些结果表明,针对人类p53产生的抗p53抗体BP53 - 12和PAb122与犬细胞中的同一分子发生交叉反应,并且p53在肿瘤发生中的作用不仅局限于人类肿瘤。我们的发现表明,应使用p53单克隆抗体组合来筛查,不仅是犬乳腺肿瘤,还有人类乳腺肿瘤,以获得更好的肿瘤预后。

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