A Distinctive Pediatric Renal Neoplasm Characterized by Epithelioid Morphology, Basement Membrane Production, Focal HMB45 Immunoreactivity, and t(6;11)(p21.1;q12) Chromosome Translocation

Argani, Pedram; Hawkins, Anita L.; Griffin, Constance A.; Goldstein, Jeffrey; Haas, Mark; Beckwith, J. Bruce; Mankinen, C. B.; Perlman, Elizabeth J.

doi:10.1016/s0002-9440(10)64680-9

Cited by 196 publications

(148 citation statements)

References 23 publications

Supporting

Mentioning

137

Contrasting

Unclassified

Order By: Relevance

“…All the cases had been earlier reported and cytogenetically confirmed. 2,3,5,[12][13][14][15][16][17] Seven cases harbored the translocation t(6;11)(p21;q12), which results in an Alpha-TFEB gene fusion and all showed confirmatory TFEB nuclear immunoreactivity as described earlier. 5 Ten cases had translocations involving Xp11.2, and all ten of these renal cell carcinomas showed confirmatory TFE3 nuclear immunoreactivity as described earlier.…”

Section: Tissue Samplessupporting

confidence: 66%

“…1,2 Several distinct gene fusions of TFE3 have been reported, 1,3,4 whereas only the specific t(6;11)(p21;q12) seems to involve the locus of TFEB. 2 These translocations result in the contribution of strong promoters that cause overexpression of the TFE3 fusion proteins or the native TFEB, such that they become detectable by immunohistochemical analysis. 5,6 Both TFE3 and TFEB are closely related members of the MiTF/TFE transcription factor family, which also includes TFEC and MiTF.…”

mentioning

confidence: 99%

See 1 more Smart Citation

Cathepsin-K immunoreactivity distinguishes MiTF/TFE family renal translocation carcinomas from other renal carcinomas

Pea²,

et al. 2009

View full text Add to dashboard Cite

The microphthalmia transcription factor/transcription factor E (TFE)-family translocation renal cell carcinomas bear specific translocations that result in overexpression of TFE3 or TFEB. TFE3 fusion gene product overexpression occurs as consequence of different translocations involving chromosome Xp11.2, whereas TFEB overexpression is the result of the specific translocation t(6;11)(p21;q12), which fuses the Alpha gene to TFEB. Both TFE3 and TFEB are closely related members of the microphthalmia transcription factor/TFE-family, which also includes TFEC and microphthalmia transcription factor. These transcription factors have overlapping transcriptional targets. Overexpression of microphthalmia transcription factor has been shown to mediate the expression of cathepsin-K in osteoclasts. We hypothesize that the overexpression of the related TFE3 fusion proteins and TFEB in translocation renal cell carcinomas may have the same effect. We studied cathepsin-K in 17 cytogenetically confirmed microphthalmia transcription factor/TFE-family translocation renal cell carcinomas. Seven cases showed a t(6;11)(p21;q12), ten cases showed translocations involving Xp11.2; five cases t(X;1)(p11;q21) resulting in a PRCC-TFE3 gene fusion; three cases t(X;1)(p11;p34) resulting in a PSF-TFE3 gene fusion, one t(X;17)(p11;q25) resulting in an ASPL-TFE3 gene fusion, and one t(X;3)(p11;q23) with an unknown TFE3 gene fusion. As control we analyzed cathepsin-K in 210 clear cell, 40 papillary, 25 chromophobe renal cell carcinomas and 30 oncocytomas. All seven TFEB translocation renal cell carcinomas were labeled for cathepsin-K. Among the cytogenetically confirmed TFE3 translocation renal cell carcinomas, 6 out of 10 were positive. None of the other renal neoplasms expressed cathepsin-K. We conclude the following: (1) cathepsin-K is consistently and strongly expressed in TFEB translocation renal cell carcinomas and in 6 of 10 TFE3 translocation renal cell carcinomas. (2) Cathepsin-K immunolabeling in both TFE3 and TFEB translocation renal cell carcinomas distinguishes these neoplasms from the more common adult renal cell carcinomas, and may be a specific marker of these neoplasms. (3) These results further support the concept that the overexpression of TFE3 or TFEB in these neoplasms activates the expression of genes normally regulated by microphthalmia transcription factor in other cell types. Keywords: cathepsin-K; TFE3; TFEB; translocation; renal cell carcinoma; immunohistochemistryThe recently described microphthalmia transcription factor/transcription factor E (MiTF/TFE) family translocation renal cell carcinomas comprise the majority of pediatric renal cell carcinomas but also occur in adults. MiTF/TFE family translocation renal cell carcinomas are characterized by specific chromosome aberrations involving the genes transcription factor E3 (TFE3) and transcription factor EB (TFEB). The TFE3 transcription factor gene maps to chromosomal region Xp11.2, whereas the TFEB transcription factor gene maps to chromosome 6p21. 1,2 Several disti...

show abstract

Section: Tissue Samplessupporting

confidence: 66%

mentioning

confidence: 99%

Cathepsin-K immunoreactivity distinguishes MiTF/TFE family renal translocation carcinomas from other renal carcinomas

Pea²,

et al. 2009

View full text Add to dashboard Cite

show abstract

“…[20][21][22][23][24][25][26][27][28][29][30][31][32] The putative oncogene, HMGIY (high mobility group protein isoforms I and Y), localized to 6p21 has been proposed to play a role in the development of a number of these neoplasms. [20][21][22][23][24][25][26][27][28][29][30][31][32][33][34] An identical t(17;17)(q12;p13) was seen in two previous studies. 7,9 Interestingly, an inversion of chromosome 17 [inv(17)(p13q11.2-12)] involving similar breakpoints was observed in case 37 of the present study (Figure 3).…”

Section: Discussionmentioning

confidence: 99%

Cytogenetic and molecular cytogenetic findings in 43 aneurysmal bone cysts: aberrations of 17p mapped to 17p13.2 by fluorescence in situ hybridization

et al. 2004

View full text Add to dashboard Cite

Aneurysmal bone cyst is a benign, cystic lesion of bone composed of blood-filled spaces separated by fibrous septa. Relatively few cases of aneurysmal bone cyst have been cytogenetically characterized, yet abnormalities of the short arm of chromosome 17 appear to be recurrent. In this study, conventional cytogenetic analysis of 43 aneurysmal bone cyst specimens from 38 patients over a 12-year period revealed clonal chromosomal abnormalities in 12 specimens. Karyotypic anomalies of 17p, including a complex translocation and inversion, were identified in eight of these 12 specimens. In an effort to further define the aberrant 17p breakpoint, fluorescence in situ hybridization (FISH) analyses were performed using a series of probe combinations spanning a 5.1 Mb region between the TP53 (17p13.1) and Miller-Dieker lissencephaly syndrome (17p13.3) gene loci. These studies revealed the critical breakpoint locus at 17p13.2, flanked proximally by an RP11-46I8, RP11-333E1, and RP11-457I18 bacterial artificial chromosome (BAC) probe cocktail and distally by an RP11-198F11 and RP11-115H24 BAC and RP5-1050D4 P1 artificial chromosome (PAC) probe cocktail. Overall, abnormalities of the 17p13.2 locus were identified by metaphase and/or interphase cell FISH analysis in 22 of 35 (63%) aneurysmal bone cyst specimens examined including 26 karyotypically normal specimens. These cytogenetic and molecular cytogenetic findings expand our knowledge of chromosomal alterations in aneurysmal bone cyst, further localize the critically involved 17p breakpoint, and provide an alternative approach (ie FISH) for detecting 17p abnormalities in nondividing cells of aneurysmal bone cysts. The latter could potentially be utilized as an adjunct in diagnostically challenging cases.

show abstract

“…Bacterial artificial chromosome (BAC) clones from the immediately flanking genomic regions of TFEB and TFE3 genes were used to generate dual color break-apart Deceptive patterns of TFEB translocation renal cell carcinoma that have been recently recognized include examples with multilocular cystic, [3] oncocytic, [4] eosinophilic papillary, [4] high-grade unclassified, [3,5] chromophobe renal cell carcinomalike, [5] tubulocystic, [6] epithelioid angiomyolipoma-like, [5] or clear cell-like [1,5] features. One example from a series of 8 tumors reported by Argani and colleagues was noted to be extensively sclerotic and ossified, [4] occurring in a 37 year-old man, similar to…”

Section: Fluorescence In Situ Hybridization (Fish)mentioning

confidence: 99%

“…[1] The unique histologic appearance of these tumors was first characterized as including large cells with clear or eosinophilic cytoplasm and a second population of smaller cells with scant cytoplasm arranged around hyaline basement membrane material, resembling rosettes. [1,2] More recently, however, other studies have found that this unique morphology is not always straightforward, and that some molecularly-confirmed TFEB rearrangement tumors may mimic clear cell renal cell carcinoma, chromophobe renal cell carcinoma, tubulocystic renal cell carcinoma, epithelioid angiomyolipoma, multilocular cystic renal cell carcinoma, or high-grade unclassified renal cell carcinoma. [3][4][5][6] One recent series included a single example that was extensively hyalinized and ossified.…”

Section: Introductionmentioning

confidence: 99%

Sclerosing TFEB -rearrangement renal cell carcinoma: a recurring histologic pattern

2017

View full text Add to dashboard Cite

A Distinctive Pediatric Renal Neoplasm Characterized by Epithelioid Morphology, Basement Membrane Production, Focal HMB45 Immunoreactivity, and t(6;11)(p21.1;q12) Chromosome Translocation

Cited by 196 publications

References 23 publications

Cathepsin-K immunoreactivity distinguishes MiTF/TFE family renal translocation carcinomas from other renal carcinomas

Cathepsin-K immunoreactivity distinguishes MiTF/TFE family renal translocation carcinomas from other renal carcinomas

Cytogenetic and molecular cytogenetic findings in 43 aneurysmal bone cysts: aberrations of 17p mapped to 17p13.2 by fluorescence in situ hybridization

Sclerosing TFEB -rearrangement renal cell carcinoma: a recurring histologic pattern

Contact Info

Product

Resources

About