Abstract
The relationship between benign uterine leiomyomas and their malignant counterparts, i.e. leiomyosarcomas and smooth muscle tumors of uncertain malignant potential (STUMP), is still poorly understood. The idea that a leiomyosarcoma could derive from a leiomyoma is still controversial. Recently MED12 mutations have been reported in uterine leiomyomas. In this study we asked whether such mutations could also be involved in leiomyosarcomas and STUMP oncogenesis. For this purpose we examined 33 uterine mesenchymal tumors by sequencing the hot-spot mutation region of MED12. We determined that MED12 is altered in 66.6% of typical leiomyomas as previously reported but also in 11% of STUMP and 20% of leiomyosarcomas. The mutated allele is predominantly expressed in leiomyomas and STUMP. Interestingly all classical leiomyomas exhibit MED12 protein expression while 40% of atypical leiomyomas, 50% of STUMP and 80% of leiomyosarcomas (among them the two mutated ones) do not express MED12. All these tumors without protein expression exhibit complex genomic profiles. No mutations and no expression loss were identified in an additional series of 38 non-uterine leiomyosarcomas. MED12 mutations are not exclusive to leiomyomas but seem to be specific to uterine malignancies. A previous study has suggested that MED12 mutations in leiomyomas could lead to Wnt/β-catenin pathway activation however our immunohistochemistry results show that there is no association between MED12 status and β-catenin nuclear/cytoplasmic localization. Collectively, our results show that subgroups of benign and malignant tumors share a common genetics. We propose here that MED12 alterations could be implicated in the development of smooth muscle tumor and that its expression could be inhibited in malignant tumors.
Highlights
Smooth muscle tumors (SMT) are the most common mesenchymal tumors of the uterus
All tumors displayed only one mutation and all Mediator complex subunit 12 (MED12) mutations are heterozygous as described by Makinen et al [17]
The two point mutations observed in LMS concerned the codon 44 and the deletion observed in Smooth muscle Tumor of Uncertain Malignant Potential (STUMP) encompassed this region
Summary
Smooth muscle tumors (SMT) are the most common mesenchymal tumors of the uterus. They encompass leiomyomas (LM), atypical LM, Smooth muscle Tumor of Uncertain Malignant Potential (STUMP) and leiomyosarcomas (LMS) [1,2,3]. STUMP tumors represent a heterogeneous group of rare tumors that cannot be histologically diagnosed as unequivocally benign or malignant, according to the World Health Organization classification [1,2,3]. Uterine LMS are aggressive tumors with a poor prognosis overall, representing 40% of uterine sarcomas and 1–3% of uterine malignancies. The histological distinction between benign and malignant SMT is based on a tree-feature morphological approach encompassing atypia, necrosis and mitotic count proposed in 1994 by Standford investigators [4].
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