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40岁及以上女性伴有卵黄囊瘤分化的恶性肿瘤的临床病理及分子分析

Clinicopathologic and Molecular Analysis of Malignant Neoplasms With Yolk Sac Tumor Differentiation in Women 40 Years of Age and Older.

作者信息

Numan Tricia A, Ronnett Brigitte M, Haley Lisa, Pallavajjala Aparna, Murry Jaclyn B, Kohn Jaden, Galbo Phillip M, Vang Russell, Rodriguez Fausto J, Kaur Harsimar, Levinson Kimberly, Lin Jeffrey, Palsgrove Doreen N

机构信息

Departments of Pathology.

Gynecology and Obstetrics, The Johns Hopkins Medical Institutions, Baltimore, MD.

出版信息

Am J Surg Pathol. 2025 Jul 1;49(7):686-700. doi: 10.1097/PAS.0000000000002389. Epub 2025 Apr 9.

Abstract

Gynecologic yolk sac tumors (YSTs) are more commonly encountered in children and young women as pure or mixed germ cell tumors and are rarely observed in older women. YSTs in older women are sometimes accompanied by a Müllerian-type carcinoma component, indicating a likely somatic rather than germ-cell origin. Studies of YSTs of germ cell and somatic types in this age group are limited. Analysis of additional pure and mixed tumors with YST differentiation could elucidate differences between these tumor subtypes and the relationship between components in mixed tumors. Clinicopathologic features of 32 malignant neoplasms with YST differentiation in women aged 40+ were analyzed. There were 11 pure YSTs, 7 mixed germ cell tumors, and 14 YSTs with a malignant non-germ cell tumor component (somatically derived yolk sac tumor [SDYST]). Targeted next-generation sequencing (NGS) was performed in 4/11 pure YSTs, 0/7 mixed germ cell tumors, and 4/14 SDYSTs. For the pure YSTs, alterations in DICER1 (1/4), PIK3R1 and PTPRT (1/4), PMS1 (1/4) , and TP53 (2/4) were identified. One other pure YST had alterations in PTEN , ARID1A , ARID1B , FGFR2 , and CTNNB1 (alterations common in endometrioid carcinoma). SDYSTs demonstrated shared alterations between both components including TP53 , KRAS , FBXW7, and KMT2C , suggesting a common origin. The findings in the pure YSTs in older women suggest that for some, the origin could be germ cell as they harbor similar alterations as those described in pure YSTs in young women, whereas in other "pure" YSTs, the molecular profile aligns with previously described SDYSTs, which suggests a SDYST with an unsampled Müllerian carcinoma component rather than a germ cell origin. In SDYSTs, shared alterations are consistent with prior studies and suggest a somatic rather than germ-cell origin.

摘要

妇科卵黄囊瘤(YSTs)在儿童和年轻女性中更常见,表现为纯或混合性生殖细胞肿瘤,在老年女性中很少见。老年女性的YSTs有时伴有米勒管型癌成分,提示可能起源于体细胞而非生殖细胞。对该年龄组生殖细胞型和体细胞型YSTs的研究有限。分析更多具有YST分化的纯性和混合性肿瘤,可能有助于阐明这些肿瘤亚型之间的差异以及混合性肿瘤中各成分之间的关系。对40岁及以上女性的32例具有YST分化的恶性肿瘤的临床病理特征进行了分析。其中有11例纯YSTs、7例混合性生殖细胞肿瘤和14例具有恶性非生殖细胞肿瘤成分的YSTs(体细胞源性卵黄囊瘤[SDYST])。对11例纯YSTs中的4例、7例混合性生殖细胞肿瘤中的0例和14例SDYSTs中的4例进行了靶向二代测序(NGS)。在纯YSTs中,发现了DICER1(1/4)、PIK3R1和PTPRT(1/4)、PMS1(1/4)以及TP53(2/4)的改变。另一例纯YST在PTEN、ARID1A、ARID1B、FGFR2和CTNNB1中有改变(这些改变在内膜样癌中常见)。SDYSTs在两个成分中都显示出共同的改变,包括TP53、KRAS、FBXW7和KMT2C,提示有共同起源。老年女性纯YSTs的研究结果表明,对于一些病例,其起源可能是生殖细胞,因为它们具有与年轻女性纯YSTs中描述的相似改变,而在其他“纯”YSTs中,分子特征与先前描述的SDYSTs一致,这表明是一种未检测到米勒管癌成分的SDYST,而非生殖细胞起源。在SDYSTs中,共同改变与先前研究一致,提示起源于体细胞而非生殖细胞。

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