PSF/SFPQ Is a Very Common Gene Fusion Partner in TFE3 Rearrangement–associated Perivascular Epithelioid Cell Tumors (PEComas) and Melanotic Xp11 Translocation Renal Cancers

Qiu Rao; Qin Shen; Qiuyuan Xia; Ziyu Wang; Biao Liu; Shanshan Shi; Qun-Li Shi; Hong-Lin Yin; Bo Wu; Sheng-bing Ye; Li Li; Jieyu Chen; Minhong Pan; Qing Li; Rui Li; Xuan Wang; Rusong Zhang; Bo Yu; Heng‐hui Ma; Zhenfeng Lu; Xiaojun Zhou

doi:10.1097/pas.0000000000000502

PSF/SFPQ Is a Very Common Gene Fusion Partner in TFE3 Rearrangement–associated Perivascular Epithelioid Cell Tumors (PEComas) and Melanotic Xp11 Translocation Renal Cancers

Qiu Rao(Nanjing University), Qin Shen(Nanjing University), Qiuyuan Xia(Nanjing University), Ziyu Wang(Nanjing University), Biao Liu(Nanjing General Hospital of Nanjing Military Command), Shanshan Shi(Nanjing General Hospital of Nanjing Military Command), Qun-Li Shi(Nanjing General Hospital of Nanjing Military Command), Hong-Lin Yin(Nanjing General Hospital of Nanjing Military Command), Bo Wu(Nanjing General Hospital of Nanjing Military Command), Sheng-bing Ye(Nanjing University), Li Li(Anhui Medical University), Jieyu Chen(Nanjing Drum Tower Hospital), Minhong Pan, Qing Li, Rui Li(Nanjing University), Xuan Wang(Nanjing General Hospital of Nanjing Military Command), Rusong Zhang(Nanjing General Hospital of Nanjing Military Command), Bo Yu(Nanjing General Hospital of Nanjing Military Command), Heng‐hui Ma(Nanjing University), Zhenfeng Lu(Nanjing University), Xiaojun Zhou(Nanjing University)

The American Journal of Surgical Pathology

August 13, 2015

10.1097/pas.0000000000000502

Cited by 102

Abstract

An increasing number of TFE3 rearrangement-associated tumors, such as TFE3 rearrangement-associated perivascular epithelioid cell tumors (PEComas), melanotic Xp11 translocation renal cancers, and melanotic Xp11 neoplasms, have recently been reported. We examined 12 such cases, including 5 TFE3 rearrangement-associated PEComas located in the pancreas, cervix, or pelvis and 7 melanotic Xp11 translocation renal cancers, using clinicopathologic, immunohistochemical, and molecular analyses. All the tumors shared a similar morphology, including a purely nested or sheet-like architecture separated by a delicate vascular network, purely epithelioid cells displaying a clear or granular eosinophilic cytoplasm, a lack of papillary structures and spindle cell or fat components, uniform round or oval nuclei containing small visible nucleoli, and, in most cases (11/12), melanin pigmentation. The levels of mitotic activity and necrosis varied. All 12 cases displayed moderately (2+) or strongly (3+) positive immunoreactivity for TFE3 and cathepsin K. One case labeled focally for HMB45 and Melan-A, whereas the others typically labeled moderately (2+) or strongly (3+) for 1 of these markers. None of the cases were immunoreactive for smooth muscle actin, desmin, CKpan, S100, or PAX8. PSF-TFE3 fusion genes were confirmed by reverse transcription polymerase chain reaction in cases (7/7) in which a novel PSF-TFE3 fusion point was identified. All of the cases displayed TFE3 rearrangement associated with Xp11 translocation. Furthermore, we developed a PSF-TFE3 fusion fluorescence in situ hybridization assay for the detection of the PSF-TFE3 fusion gene and detected it in all 12 cases. Clinical follow-up data were available for 7 patients. Three patients died, and 2 patients (cases 1 and 3) remained alive with no evidence of disease after initial resection. Case 2 experienced recurrence and remained alive with disease. Case 5, a recent case, remained alive with extensive abdominal cavity metastases. Our data suggest that these tumors belong to a single clinicopathologic spectrum and expand the known characteristics of TFE3 rearrangement-associated tumors.

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