LPCAT1-TERT fusions are uniquely recurrent in epithelioid trophoblastic tumors and positively regulate cell growth.

Gavin R Oliver,Ezequiel J Tolosa,Sarah Kerr,Jesse S Voss,Amy A Swanson,John K Schoolmeester,Jan B Egan,Sofia Marcano-Bonilla,Shannon M Knight,Anthony G Bilyeu,Eriko Iguchi,Ema Veras,Nicole L Hoppman,Jonathan Quist,Eric W Klee,Numrah Fadra,Naresh Prodduturi,Jin Zhang,Jin Jen,Matthew S Block ,Tanya L Schwab ,Michael A Zimmerman ,Ashley N Sigafoos ,Martín E Fernández-Zapico ,Raúl Urrutia ,Remaa Al-Safi

doi:10.1371/journal.pone.0250518

Abstract

Gestational trophoblastic disease (GTD) is a heterogeneous group of lesions arising from placental tissue. Epithelioid trophoblastic tumor (ETT), derived from chorionic-type trophoblast, is the rarest form of GTD with only approximately 130 cases described in the literature. Due to its morphologic mimicry of epithelioid smooth muscle tumors and carcinoma, ETT can be misdiagnosed. To date, molecular characterization of ETTs is lacking. Furthermore, ETT is difficult to treat when disease spreads beyond the uterus. Here using RNA-Seq analysis in a cohort of ETTs and other gestational trophoblastic lesions we describe the discovery of LPCAT1-TERT fusion transcripts that occur in ETTs and coincide with underlying genomic deletions. Through cell-growth assays we demonstrate that LPCAT1-TERT fusion proteins can positively modulate cell proliferation and therefore may represent future treatment targets. Furthermore, we demonstrate that TERT upregulation appears to be a characteristic of ETTs, even in the absence of LPCAT1-TERT fusions, and that it appears linked to copy number gains of chromosome 5. No evidence of TERT upregulation was identified in other trophoblastic lesions tested, including placental site trophoblastic tumors and placental site nodules, which are thought to be the benign chorionic-type trophoblast counterpart to ETT. These findings indicate that LPCAT1-TERT fusions and copy-number driven TERT activation may represent novel markers for ETT, with the potential to improve the diagnosis, treatment, and outcome for women with this rare form of GTD.

Highlights

Gestational trophoblastic disease (GTD) is a heterogeneous group of lesions that includes both neoplastic and non-neoplastic entities
LPCAT1-TERT fusion transcripts occur in epithelioid trophoblastic tumors
Samples were collected for three epithelioid trophoblastic tumor (ETT), four placental site nodule (PSN) and two placental site trophoblastic tumor (PSTT) (Table 1)

Summary

Introduction

Gestational trophoblastic disease (GTD) is a heterogeneous group of lesions that includes both neoplastic and non-neoplastic entities. As defined by the 2014 WHO Classification of Tumors of Female Reproductive Organs [1], choriocarcinoma, placental site trophoblastic tumor (PSTT) and epithelioid trophoblastic tumor (ETT) encompass the neoplasms [2], whereas exaggerated implantation/placental site and placental site nodule (PSN) are non-neoplastic counterparts. ETT, the rarest form of GTD [4, 5], is composed of chorionic-type intermediate trophoblast that has potential for metastasis. PSN is composed of chorionic-type intermediate trophoblast, it is benign. Mixed histologies are observed [6], and recently lesions possessing features between those of PSN and ETT have been classified as atypical PSNs [3]. Atypical PSNs are considered intermediate lesions in the spectrum of PSN and ETT. It has been proposed that ETT and PSTT might evolve from a previous PSN [8,9,10]

Methods

Results

Conclusion