Clinicopathological Findings on 28 Cases with XP11.2 Renal Cell Carcinoma.


Journal

Pathology oncology research : POR
ISSN: 1532-2807
Titre abrégé: Pathol Oncol Res
Pays: Switzerland
ID NLM: 9706087

Informations de publication

Date de publication:
Oct 2020
Historique:
received: 30 08 2019
accepted: 30 12 2019
pubmed: 20 1 2020
medline: 13 7 2021
entrez: 20 1 2020
Statut: ppublish

Résumé

Xp11.2 translocation carcinoma is a distinct subtype of renal cell carcinoma characterized by translocations involving the TFE3 gene. Our study included the morphological, immunohistochemical and clinicopathological examination of 28 Xp11.2 RCCs. The immunophenotype has been assessed by using CA9, CK7, CD10, AMACR, MelanA, HMB45, Cathepsin K and TFE3 immunostainings. The diagnosis was confirmed by TFE3 break-apart FISH in 25 cases. The ages of 13 male and 15 female patients, without underlying renal disease or having undergone chemotherapy ranged from 8 to 72. The mean size of the tumors was 78.5 mm. Forty-three percent of patients were diagnosed in the pT3/pT4 stage with distant metastasis in 6 cases. Histological appearance was branching-papillary composed of clear cells with voluminous cytoplasm in 13 and variable in 15 cases, including one tumor with anaplastic carcinoma and another with rhabdoid morphology. Three tumors were labeled with CA9, while CK7 was negative in all cases. Diffuse CD10 reaction was observed in 17 tumors and diffuse AMACR positivity was described in 14 tumors. The expression of melanocytic markers and Cathepsin K were seen only in 7 and 6 cases, respectively. TFE3 immunohistochemistry displayed a positive reaction in 26/28 samples. TFE3 rearrangement was detected in all the analyzed cases (25/25), including one with the loss of the entire labeled break-point region. The follow-up time ranged from 2 to 300 months, with 7 cancer-related deaths. In summary, Xp11.2 carcinoma is an uncommon form of renal cell carcinoma with a variable histomorphology and rather aggressive clinical course.

Identifiants

pubmed: 31955345
doi: 10.1007/s12253-019-00792-0
pii: 10.1007/s12253-019-00792-0
pmc: PMC7471254
doi:

Substances chimiques

Basic Helix-Loop-Helix Leucine Zipper Transcription Factors 0
Biomarkers, Tumor 0
TFE3 protein, human 0

Types de publication

Journal Article

Langues

eng

Sous-ensembles de citation

IM

Pagination

2123-2133

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Auteurs

Levente Kuthi (L)

Department of Pathology, University of Szeged, 1 Állomás Street, Szeged, H-6725, Hungary. kuthi.levente@med.u-szeged.hu.

Áron Somorácz (Á)

2nd Department of Pathology, Semmelweis University, Budapest, Hungary.

Tamás Micsik (T)

1st Department of Pathology and Experimental Cancer Research, Semmelweis University, Budapest, Hungary.

Alex Jenei (A)

Department of Pathology, University of Szeged, 1 Állomás Street, Szeged, H-6725, Hungary.

Adrienn Hajdu (A)

Department of Pathology, University of Szeged, 1 Állomás Street, Szeged, H-6725, Hungary.

István Sejben (I)

Department of Pathology, Bács-Kiskun County Teaching Hospital, Kecskemét, Hungary.

Dániel Imre (D)

Department of Pathology, Hetényi Géza County Hospital, Szolnok, Hungary.

Boglárka Pósfai (B)

Department of Oncotherapy, University of Szeged, Szeged, Hungary.

Katalin Kóczián (K)

Surgical and Molecular Tumor Pathology Centre, National Institute of Oncology, Budapest, Hungary.

Dávid Semjén (D)

Department of Pathology, Clinical Center and Medical School, University of Pécs, Pécs, Hungary.

Zoltán Bajory (Z)

Department of Urology, University of Szeged, Szeged, Hungary.

Janina Kulka (J)

2nd Department of Pathology, Semmelweis University, Budapest, Hungary.

Béla Iványi (B)

Department of Pathology, University of Szeged, 1 Állomás Street, Szeged, H-6725, Hungary.

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