Using short tandem repeat analysis for choriocarcinoma diagnosis: a case series

Xiaofei Zhang; Kai Yan; Jianhua Chen; Xing Xie

doi:10.1186/s13000-019-0866-5

Diagnostic Pathology (Aug 2019)

Using short tandem repeat analysis for choriocarcinoma diagnosis: a case series

Xiaofei Zhang,
Kai Yan,
Jianhua Chen,
Xing Xie

Affiliations

Xiaofei Zhang: Department of Surgical Pathology, Women’s Hospital, School of Medicine, Zhejiang University
Kai Yan: Department of Reproductive genomics, Women’s Hospital, School of Medicine, Zhejiang University
Jianhua Chen: Department of Surgical Pathology, Women’s Hospital, School of Medicine, Zhejiang University
Xing Xie: Department of Gynecologic Oncology, Women’s Hospital, School of Medicine, Zhejiang University

DOI: https://doi.org/10.1186/s13000-019-0866-5
Journal volume & issue: Vol. 14, no. 1
pp. 1 – 13

Abstract

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Abstract Background Choriocarcinoma is a highly aggressive, malignant trophoblastic neoplasm that can be gestational or non-gestational in origin. Accurate discrimination between these two subtypes, the causative pregnancy type, and the pregnancy-to-treatment interval for gestational choriocarcinoma are vital for clinical management. Methods Fifteen choriocarcinomas were genotyped using multiplex fluorescent polymerase chain reaction amplification of 15 short tandem repeat (STR) loci and the amelogenin locus (XY determination). Genotype patterns at each locus from tumoral and maternal tissues were compared, and any prior or concurrent mole/placenta was also compared when available. According to STR results showing the presence or absence of the paternal chromosomal complement, the gestational or non-gestational origin of the tumor and the nature of the causative pregnancy was identified. Results Fourteen tumors were gestational. Of these, seven were androgenetic/homozygous XX, and two were androgenetic/heterozygous XX, indicating that the causative pregnancies were molar pregnancies. Among the nine molar pregnancies, five were of the occult type. A menopausal patient developed a tumor from a mole that occurred seven years ago, identified by the genetically identical allele from the tumor and prior mole. One tumor originating from a previous mole was interrupted by term delivery. Two tumors found eight weeks postpartum were identified as originating from a prior occult mole. A pelvic choriocarcinoma was separated from a genetically distinct third trimester intrauterine placenta. Five gestational tumors were biparental: 2 XX, 3 XY. Of three ovarian tumors, two were confirmed gestational (1 androgenetic/homozygous XX; 1 biparental XY), and one was an ovarian tumor (XX) with a complete match of the genotype for all 15 loci, therefore ascertaining its non-gestational origin. Conclusion Gestational choriocarcinoma can originate in an androgenetic or biparental manner. The majority are androgenetic/homozygous XX, while a large number of them might be occult molar pregnancies. The origin of ectopic androgenetic choriocarcinoma with concurrent intrauterine placenta might be from either dispermic twin gestation (mole and coexistent nonmolar fetus) or an antecedent molar pregnancy. Choriocarcinoma shortly postpartum might not be associated with the last placenta. STR analysis can be useful in distinguishing gestational choriocarcinoma from non-gestational, as well as the causative pregnancy, and serve as a helpful examination tool for guiding clinical management.

Published in Diagnostic Pathology

ISSN: 1746-1596 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Pathology
Website: https://diagnosticpathology.biomedcentral.com/

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