首页> 外文期刊>The Journal of investigative dermatology. >Second Primary Cancers in Patients with Invasive and In Situ Squamous Cell Skin Carcinoma, Kaposi Sarcoma, and Merkel Cell Carcinoma: Role for Immune Mechanisms?
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Second Primary Cancers in Patients with Invasive and In Situ Squamous Cell Skin Carcinoma, Kaposi Sarcoma, and Merkel Cell Carcinoma: Role for Immune Mechanisms?

机译:侵袭性和原位鳞状细胞皮肤癌,Kaposi Sarcoma和Merkel细胞癌的第二次癌症:免疫机制的作用?

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摘要

Second primary cancers (SPCs) are becoming a common cancer entity, which may interfere with survival in relatively benign first primary cancers. We examined the hypothesis that immune dysfunction may contribute to SPCs by assessing SPCs associated with known immune responsive skin cancers, invasive and in situ squamous cell carcinoma, Kaposi sarcoma, and Merkel cell carcinoma. Cancers were identified from the Swedish Cancer Registry from the year 1958 to 2015. Standardized relative risks were calculated bidirectionally for any SPC after skin cancer and for skin cancer as SPC. Over 80,000 first primary cancers were identified for each invasive and in situ squamous cell carcinoma of the skin. Bidirectional increased risks were observed for 26 cancers associated with invasive skin cancer; the Spearman rank correlation was 0.72 (P = 4.6 x 10(-5)). The highest bidirectional relative risks were for invasive and in situ skin cancer as SPCs (14.59 and 16.71, respectively). Remarkably high risks for second in situ squamous cell carcinoma of the skin were found after Kaposi sarcoma (685.68) and Merkel cell carcinoma (117.23). The high systematic bidirectional risks between immune responsive skin cancers and most other cancers suggest that immune suppression is a key mechanism contributing to an increased risk of SPCs.
机译:第二次主要癌症(SPC)正在成为常见的癌症实体,这可能会干扰相对良性的第一原癌症中的存活。我们检查了通过评估与已知免疫应答皮肤癌,侵袭性和原位鳞状细胞癌,Kaposi Sarcoma和Merkel细胞癌相关的SPC来对SPC有助于SPC的假设。从1958年至2015年从瑞典癌症登记处鉴定了癌症。标准化的相对风险被双向对皮肤癌和皮肤癌作为SPC的任何SPC进行双向计算。针对皮肤的每种侵入性和原位鳞状细胞癌鉴定超过80,000次原发性癌症。观察到与侵袭性皮肤癌相关的26个癌症观察到双向的风险; Spearman等级相关是0.72(p = 4.6×10(-5))。最高的双向相对风险是用于侵入性的和原位皮肤癌作为SPCS(分别为14.59和16.71)。在Kaposi Sarcoma(685.68)和Merkel细胞癌(117.23)后发现皮肤的第二次鳞状细胞癌的高风险。免疫应答皮肤癌和大多数其他癌症之间的高系统双向风险表明免疫抑制是促进SPC的风险增加的关键机制。

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