PD-L1和p53在口咽鳞状细胞癌中的表达与人乳头瘤病毒状态的关系

D. Sh. Polatova, A. Yu. Madaminov, A. V. Savkin, A. I. Nurzhabov, N. K. Asamedinov, D. A. Ibragimova, R. R. Davletov, S. K. Nasirov
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摘要

介绍。高危人乳头瘤病毒(Hpv),特别是基因型16,导致口咽鳞状细胞癌(OSCC)。在大约70%的扁桃体淋巴组织或舌底的肿瘤中可以检测到它。由于Hpv阳性OSCC的数量增加,Hpv状态被认为是OSCC临床结果的标志。p16INk4a免疫组化分析检测简单、成本低、可靠、灵敏度高,广泛应用于Hpv状态检测。的目标。目的:探讨程序性死亡配体1 (pD-L1)和p53表达与间接Hpv标志物p16INk4a在OSCC患者中的存在之间的关系。材料和方法。该研究包括76名OSCC т1-4N0-3m0患者,他们在2015年至2020年期间在共和党肿瘤和放射学专业科学和实用医学中心(n = 37)及其塔什干分支机构(n = 39)接受治疗。对所有选定的患者进行回顾性免疫组化分析,检测石蜡块中福尔马林固定的肿瘤样本中p16INk4a、pD-L1和 p53 - 3的存在。在我们的工作中,p16INk4a的免疫组化检查是确定Hpv状态的唯一相关工具。为了加强其预后意义,我们使用了在癌变转化和OSCC进展中起重要作用的额外分子标志物pD-L1和p53。结果。免疫组化分析结果显示,46%(6/13)的患者p16INk4a过表达并伴有pD-L1阳性反应;突变型p53无阳性表达。野生型p53仅在1例(3%)病例中被鉴定为p16INk4a过表达。结论。由3个分子标记(p16INk4a、pD-L1和53)组成的小组可能在准确预后、风险分层和了解OSCC分子特征方面开辟新的领域。反过来,这将有助于临床医生选择个体治疗策略,以降低治疗升级和优化结果。
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PD-L1 and p53 expression in squamous cell carcinoma of the oropharynx depending on human papilloma virus status
Introduction. High-risk human papilloma virus (Hpv), especially genotype 16, causes oropharyngeal squamous cell carcinoma (OSCC). It is detected in about 70 % of tumors developing from lymphoid tissue of the tonsils or the base of the tongue. Due to the increased number of Hpv-positive OSCC, Hpv status is considered a marker of OSCC clinical outcome. Easy testing, low cost, reliability, and high sensitivity of immunohistochemical analysis for p16INk4a allowed to widely use this method for Hpv status determination. Aim. To determine the association between programmed death-ligand 1 (pD-L1) and p53 expression and presence of indirect Hpv marker – p16INk4a – in patients with OSCC. Materials and methods . The study included 76 patients with OSCC т1–4N0–3m0 who received treatment at the Republican Specialized Scientific and practical medical Center of Oncology and Radiology (n = 37) and its Tashkent branch (n = 39) between 2015 and 2020. for all selected patients, retrospective immunohistochemical analysis for the presence of p16INk4a, pD-L1 and р53 in tumor samples fixed with formalin in paraffin blocks was performed. In our work, immunohistochemical examination for p16INk4a was the only relevant tool for Hpv status determination. To reinforce its prognostic significance, we used additional molecular markers pD-L1 and p53 which play an important role in carcinogenic transformation and OSCC progression. Results. The results of immunohistochemical analysis showed that p16INk4a overexpression was accompanied by positive pD-L1 reaction in 46 % (6/13) of cases; there were no cases of positive expression of mutant type p53. wild type p53 was identified in only 1 (3 %) case in combination with p16INk4a overexpression. Conclusion. The developed panel consisting of 3 molecular markers (p16INk4a, pD-L1 and р53) may open new horizons in accurate prognosis, risk stratification and understanding of OSCC molecular signature. This, in turn, will help clinicians in selection of individual therapy strategies for treatment de-escalation and outcome optimization.
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