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双重困扰:同时性和异时性原发性肿瘤使 ctHPV DNA 监测复杂化。

Double trouble: Synchronous and metachronous primaries confound ctHPVDNA monitoring.

机构信息

Department of Otolaryngology - Head and Neck Surgery, Massachusetts Eye and Ear, Boston, Massachusetts, USA.

Harvard Medical School, Boston, Massachusetts, USA.

出版信息

Head Neck. 2023 Jun;45(6):E25-E30. doi: 10.1002/hed.27378. Epub 2023 Apr 20.

Abstract

BACKGROUND

Human papillomavirus-associated head and neck squamous cell carcinoma (HPV + HNSCC) occurs in the oropharynx (HPV + OPSCC), sinonasal cavity (HPV + SNSCC), and nasopharynx (HPV + NPC). Circulating tumor HPV DNA (ctHPVDNA) is an accurate tool for diagnosis, treatment monitoring, and recurrence detection. An emerging challenge with ctHPVDNA is that ~7.4% of HPV + HNSCC patients develop synchronous or metachronous HPV+ primaries, which could confound ctHPVDNA monitoring.

METHODS

We describe a 65-year-old patient with T2N1M0 HPV16 + OPSCC and a 55-year-old patient with T2N2M0 HPV16 + OPSCC. Both patients were enrolled in our prospective observational ctHPVDNA study with longitudinal blood collections throughout treatment. Both patients developed multiple HPV+ primaries.

RESULTS

Detailed discussion of the patients' treatment courses, the subsequent diagnoses of their second HPV+ primaries, and their ctHPVDNA monitoring is presented.

CONCLUSIONS

As ctHPVDNA use becomes more prevalent, it is important to recognize that an increase in ctHPVDNA can come not only from the primary tumor or metastatic clones, but also from synchronous or metachronous second primaries.

摘要

背景

人乳头瘤病毒相关的头颈部鳞状细胞癌(HPV+ HNSCC)发生在口咽(HPV+ OPSCC)、鼻腔鼻窦(HPV+ SNSCC)和鼻咽(HPV+ NPC)。循环肿瘤 HPV DNA(ctHPVDNA)是一种用于诊断、治疗监测和复发检测的准确工具。ctHPVDNA 面临的一个新挑战是,约 7.4%的 HPV+ HNSCC 患者会出现同步或异时性 HPV+ 原发性肿瘤,这可能会干扰 ctHPVDNA 监测。

方法

我们描述了 2 例患者,例 1 为 65 岁的 T2N1M0 HPV16+ OPSCC 患者,例 2 为 55 岁的 T2N2M0 HPV16+ OPSCC 患者。这 2 例患者均被纳入我们的前瞻性观察性 ctHPVDNA 研究,在整个治疗过程中进行纵向血液采集。这 2 例患者均出现了多个 HPV+原发性肿瘤。

结果

详细讨论了患者的治疗过程、随后诊断出的第二例 HPV+原发性肿瘤以及他们的 ctHPVDNA 监测情况。

结论

随着 ctHPVDNA 的应用越来越普遍,重要的是要认识到,ctHPVDNA 的增加不仅来自原发性肿瘤或转移性克隆,还可能来自同步或异时性的第二原发性肿瘤。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1f1f/10236316/5f5f4db3e82e/nihms-1892807-f0001.jpg

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