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异常迁移能否解释异时性生殖细胞肿瘤?

Could Aberrant Migration Explain Metachronous Germ Cell Tumors?

机构信息

Institut d'Hématologie et d'Oncologie Pédiatrique, Lyon, France.

Hospices Civils de Lyon, Department of Pathology, Lyon, France.

出版信息

Cancer Invest. 2021 Feb;39(2):195-201. doi: 10.1080/07357907.2020.1828447. Epub 2020 Nov 6.

DOI:10.1080/07357907.2020.1828447
PMID:33017201
Abstract

BACKGROUND

Extragonadal germ cell tumors (GCTs) are thought to arise as a result of local transformation of primordial gonadal cells (PGCs) that become misplaced during embryogenesis. With the exception of bilateral testis tumors, metachronous GCT (i.e., occurring at a site classically described for primary GCTs) are rare events.

PATIENTS AND METHODS

The clinical, radiological, and molecular data (if available) of patients with metachronous GCT were analyzed.

RESULTS

Three Caucasian males were identified: case 1 presented with a pineal germinoma 19 years after a mediastinal seminoma that had been treated with chemotherapy, case 2 presented with a pineal non-seminomatous GCT (NSGCT) that occurred three years after a mediastinal seminoma treated with chemotherapy, and case 3 presented with a mediastinal seminoma concomitant with a suprasellar germinoma that occurred two years after a stage I testicular NSGCT treated exclusively with surgery. None of these patients had a positive family history or disorder of sex development. Molecular data were available for cases 2 and 3. In case 2, a gene biallelic inactivation in the second tumor suggested chemoresistance to cisplatin. This was further confirmed by tumor progression during second-line treatment. In case 3, the molecular analysis revealed different profiles in the three tumors, thus suggesting distinct tumor cell origins.

CONCLUSION

These rare cases should alert clinicians of the possibility of multiple GCTs that should not be considered to be relapses. The underlying physiopathology is unknown, but multiple PGC mismigrations is a likely cause. Initial treatment with cisplatin may select chemo-resistant clones, thereby making the subsequent treatment more of a challenge.

摘要

背景

性腺外生殖细胞肿瘤(GCT)被认为是由于胚胎发生过程中原始生殖细胞(PGC)位置不当而导致局部转化而产生的。除了双侧睾丸肿瘤外,异时性 GCT(即在经典描述原发性 GCT 的部位发生)是罕见事件。

患者和方法

分析了异时性 GCT 患者的临床、影像学和分子数据(如果有)。

结果

确定了 3 名白人男性:病例 1 表现为松果体生殖细胞瘤,19 年前曾患有纵隔精原细胞瘤,接受过化疗;病例 2 表现为松果体非精原细胞瘤 GCT(NSGCT),3 年前曾患有纵隔精原细胞瘤,接受过化疗;病例 3 表现为纵隔精原细胞瘤同时伴有颅咽管瘤,2 年前曾患有 I 期睾丸 NSGCT,仅接受手术治疗。这些患者均无阳性家族史或性发育障碍。病例 2 和 3 有分子数据。在病例 2 中,第二个肿瘤中基因的双等位基因失活提示对顺铂的化疗耐药。这通过二线治疗期间肿瘤进展得到进一步证实。在病例 3 中,分子分析显示三个肿瘤的图谱不同,因此提示肿瘤细胞起源不同。

结论

这些罕见病例应提醒临床医生注意存在多个 GCT 的可能性,不应将其视为复发。潜在的病理生理学尚不清楚,但多个 PGC 迁移错误可能是一个原因。初始顺铂治疗可能会选择化疗耐药克隆,从而使后续治疗更加具有挑战性。

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