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猫鼻平面鳞状细胞癌中 p16 CDKN2A 蛋白免疫染色的存在与生存时间的延长和乳头瘤病毒 DNA 的存在相关。

The presence of p16 CDKN2A protein immunostaining within feline nasal planum squamous cell carcinomas is associated with an increased survival time and the presence of papillomaviral DNA.

机构信息

Institute of Veterinary, Animal and Biomedical Sciences, Massey University, Palmerston North 4442, New Zealand.

出版信息

Vet Pathol. 2013 Mar;50(2):269-73. doi: 10.1177/0300985812452582. Epub 2012 Jun 29.

Abstract

In humans, oral SCCs are either caused by papillomavirus (PV) infection or by other carcinogens such as tobacco. As these 2 groups of SCCs have different causes they also have different clinical behaviors. Immunostaining using anti-p16(CDKN2A) protein (p16) antibodies is used to indicate a PV etiology in human oral SCCs and p16-positive SCCs have a more favorable prognosis. The present study investigated whether p16 immunostaining within feline nasal planum SCCs was similarly associated with the presence of PV DNA and with a longer survival time. Intense p16 immunostaining was visible in 32 of 51 (63%) SCCs. In 30 cats with nonexcised SCCs, cats with p16-positive neoplasms had a longer estimated mean survival time (643 days) than cats with p16-negative SCCs (217 days, P = .013). Papillomavirus DNA was amplified more frequently from p16-positive nasal planum SCCs (28 of 32) than p16-negative SCCs (5 of 19, P < .001). The different survival times in cats with p16-positive and p16-negative SCCs suggests that p16 could be a useful prognostic indicator in these common feline cancers. As the clinical behavior of the SCCs can be subdivided using p16 immunostaining, the 2 groups of SCCs may be caused by different factors, supporting a PV etiology in a proportion of feline nasal planum SCCs.

摘要

在人类中,口腔 SCC 要么由乳头瘤病毒 (PV) 感染引起,要么由其他致癌物(如烟草)引起。由于这两组 SCC 的病因不同,它们的临床行为也不同。使用抗 p16(CDKN2A) 蛋白 (p16) 抗体的免疫染色用于指示人类口腔 SCC 中的 PV 病因,p16 阳性 SCC 具有更好的预后。本研究调查了猫鼻平面 SCC 中 p16 免疫染色是否与 PV DNA 的存在以及更长的生存时间有关。在 51 个 SCC 中,有 32 个(63%)可见强烈的 p16 免疫染色。在 30 只未切除 SCC 的猫中,p16 阳性肿瘤的猫估计平均存活时间(643 天)长于 p16 阴性 SCC 的猫(217 天,P =.013)。p16 阳性鼻平面 SCC(28 个中的 32 个)比 p16 阴性 SCC(19 个中的 5 个)更频繁地扩增出 PV DNA(P <.001)。p16 阳性和 p16 阴性 SCC 猫的不同存活时间表明,p16 可能是这些常见猫科癌症的有用预后指标。由于 SCC 的临床行为可以使用 p16 免疫染色进行细分,因此 SCC 的两组可能由不同的因素引起,这支持了一部分猫鼻平面 SCC 的 PV 病因。

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