Genotype-phenotype features of germline variants of the TMEM127 pheochromocytoma susceptibility gene: A 10-year update

Gustavo Armaiz-Pena; Shahida K. Flores; Zi Ming Cheng; Xhingyu Zhang; Emmanuel Esquivel; Natalie Poullard; Anusha Vaidyanathan; Qianqian Liu; Joel Michalek; Alfredo A. Santillan-Gomez; Michael Liss; Sara Ahmadi; Daniel Katselnik; Enrique Maldonado; Sarimar Agosto Salgado; Camilo Jimenez; Lauren Fishbein; Oksana Hamidi; Tobias Else; Ron Lechan; Art S. Tischler; Diana E. Benn; Trisha Dwight; Rory Clifton-Bligh; Gabriela Sanso; Marta Barontini; Deepa Vincent; Neil Aronin; Bernadette Biondi; Maureen Koops; Elizabeth Bowhay-Carnes; Anne Paule Gimenez-Roqueplo; Andrea Alvarez-Eslava; Jan M. Bruder; Mio Kitano; Nelly Burnichon; Yanli Ding; Patricia L.M. Dahia

doi:10.1210/clinem/dgaa741

Genotype-phenotype features of germline variants of the TMEM127 pheochromocytoma susceptibility gene: A 10-year update

Gustavo Armaiz-Pena, Shahida K. Flores, Zi Ming Cheng, Xhingyu Zhang, Emmanuel Esquivel, Natalie Poullard, Anusha Vaidyanathan, Qianqian Liu, Joel Michalek, Alfredo A. Santillan-Gomez, Michael Liss, Sara Ahmadi, Daniel Katselnik, Enrique Maldonado, Sarimar Agosto Salgado, Camilo Jimenez, Lauren Fishbein, Oksana Hamidi, Tobias Else, Ron LechanArt S. Tischler, Diana E. Benn, Trisha Dwight, Rory Clifton-Bligh, Gabriela Sanso, Marta Barontini, Deepa Vincent, Neil Aronin, Bernadette Biondi, Maureen Koops, Elizabeth Bowhay-Carnes, Anne Paule Gimenez-Roqueplo, Andrea Alvarez-Eslava, Jan M. Bruder, Mio Kitano, Nelly Burnichon, Yanli Ding, Patricia L.M. Dahia

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Abstract

Purpose: This work aimed to evaluate genotype-phenotype associations in individuals carrying germline variants of transmembrane protein 127 gene (TMEM127), a poorly known gene that confers susceptibility to pheochromocytoma (PHEO) and paraganglioma (PGL). Design: Data were collected from a registry of probands with TMEM127 variants, published reports, and public databases. Main Outcome Analysis: Clinical, genetic, and functional associations were determined. Results: The cohort comprised 110 index patients (111 variants) with a mean age of 45 years (range, 21-84 years). Females were predominant (76 vs 34, P <. 001). Most patients had PHEO (n = 94; 85.5%), although PGL (n = 10; 9%) and renal cell carcinoma (RCC, n = 6; 5.4%) were also detected, either alone or in combination with PHEO. One-third of the cases had multiple tumors, and known family history was reported in 15.4%. Metastatic PHEO/PGL was rare (2.8%). Epinephrine alone, or combined with norepinephrine, accounted for 82% of the catecholamine profiles of PHEO/PGLs. Most variants (n = 63) occurred only once and 13 were recurrent (2-12 times). Although nontruncating variants were less frequent than truncating changes overall, they were predominant in non-PHEO clinical presentations (36% PHEO-only vs 69% other, P <. 001) and clustered disproportionately within transmembrane regions (P <. 01), underscoring the relevance of these domains for TMEM127 function. Integration of clinical and previous experimental data supported classification of variants into 4 groups based on mutation type, localization, and predicted disruption. Conclusions: Patients with TMEM127 variants often resemble sporadic nonmetastatic PHEOs. PGL and RCC may also co-occur, although their causal link requires further evaluation. We propose a new classification to predict variant pathogenicity and assist with carrier surveillance.

Original language	English (US)
Pages (from-to)	E350-E364
Journal	Journal of Clinical Endocrinology and Metabolism
Volume	106
Issue number	1
DOIs	https://doi.org/10.1210/clinem/dgaa741
State	Published - Jan 1 2021

Keywords

Genotype-phenotype association
Paraganglioma
Pheochromocytoma
TMEM127
Tumor suppressor gene

ASJC Scopus subject areas

Endocrinology, Diabetes and Metabolism
Biochemistry
Endocrinology
Clinical Biochemistry
Biochemistry, medical

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10.1210/clinem/dgaa741

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Armaiz-Pena, G., Flores, S. K., Cheng, Z. M., Zhang, X., Esquivel, E., Poullard, N., Vaidyanathan, A., Liu, Q., Michalek, J., Santillan-Gomez, A. A., Liss, M., Ahmadi, S., Katselnik, D., Maldonado, E., Salgado, S. A., Jimenez, C., Fishbein, L., Hamidi, O., Else, T., ... Dahia, P. L. M. (2021). Genotype-phenotype features of germline variants of the TMEM127 pheochromocytoma susceptibility gene: A 10-year update. Journal of Clinical Endocrinology and Metabolism, 106(1), E350-E364. https://doi.org/10.1210/clinem/dgaa741

Armaiz-Pena, G, Flores, SK, Cheng, ZM, Zhang, X, Esquivel, E, Poullard, N, Vaidyanathan, A, Liu, Q, Michalek, J, Santillan-Gomez, AA, Liss, M, Ahmadi, S, Katselnik, D, Maldonado, E, Salgado, SA, Jimenez, C, Fishbein, L, Hamidi, O, Else, T, Lechan, R, Tischler, AS, Benn, DE, Dwight, T, Clifton-Bligh, R, Sanso, G, Barontini, M, Vincent, D, Aronin, N, Biondi, B, Koops, M, Bowhay-Carnes, E, Gimenez-Roqueplo, AP, Alvarez-Eslava, A, Bruder, JM, Kitano, M, Burnichon, N, Ding, Y & Dahia, PLM 2021, 'Genotype-phenotype features of germline variants of the TMEM127 pheochromocytoma susceptibility gene: A 10-year update', Journal of Clinical Endocrinology and Metabolism, vol. 106, no. 1, pp. E350-E364. https://doi.org/10.1210/clinem/dgaa741

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title = "Genotype-phenotype features of germline variants of the TMEM127 pheochromocytoma susceptibility gene: A 10-year update",

abstract = "Purpose: This work aimed to evaluate genotype-phenotype associations in individuals carrying germline variants of transmembrane protein 127 gene (TMEM127), a poorly known gene that confers susceptibility to pheochromocytoma (PHEO) and paraganglioma (PGL). Design: Data were collected from a registry of probands with TMEM127 variants, published reports, and public databases. Main Outcome Analysis: Clinical, genetic, and functional associations were determined. Results: The cohort comprised 110 index patients (111 variants) with a mean age of 45 years (range, 21-84 years). Females were predominant (76 vs 34, P <. 001). Most patients had PHEO (n = 94; 85.5%), although PGL (n = 10; 9%) and renal cell carcinoma (RCC, n = 6; 5.4%) were also detected, either alone or in combination with PHEO. One-third of the cases had multiple tumors, and known family history was reported in 15.4%. Metastatic PHEO/PGL was rare (2.8%). Epinephrine alone, or combined with norepinephrine, accounted for 82% of the catecholamine profiles of PHEO/PGLs. Most variants (n = 63) occurred only once and 13 were recurrent (2-12 times). Although nontruncating variants were less frequent than truncating changes overall, they were predominant in non-PHEO clinical presentations (36% PHEO-only vs 69% other, P <. 001) and clustered disproportionately within transmembrane regions (P <. 01), underscoring the relevance of these domains for TMEM127 function. Integration of clinical and previous experimental data supported classification of variants into 4 groups based on mutation type, localization, and predicted disruption. Conclusions: Patients with TMEM127 variants often resemble sporadic nonmetastatic PHEOs. PGL and RCC may also co-occur, although their causal link requires further evaluation. We propose a new classification to predict variant pathogenicity and assist with carrier surveillance.",

keywords = "Genotype-phenotype association, Paraganglioma, Pheochromocytoma, TMEM127, Tumor suppressor gene",

author = "Gustavo Armaiz-Pena and Flores, {Shahida K.} and Cheng, {Zi Ming} and Xhingyu Zhang and Emmanuel Esquivel and Natalie Poullard and Anusha Vaidyanathan and Qianqian Liu and Joel Michalek and Santillan-Gomez, {Alfredo A.} and Michael Liss and Sara Ahmadi and Daniel Katselnik and Enrique Maldonado and Salgado, {Sarimar Agosto} and Camilo Jimenez and Lauren Fishbein and Oksana Hamidi and Tobias Else and Ron Lechan and Tischler, {Art S.} and Benn, {Diana E.} and Trisha Dwight and Rory Clifton-Bligh and Gabriela Sanso and Marta Barontini and Deepa Vincent and Neil Aronin and Bernadette Biondi and Maureen Koops and Elizabeth Bowhay-Carnes and Gimenez-Roqueplo, {Anne Paule} and Andrea Alvarez-Eslava and Bruder, {Jan M.} and Mio Kitano and Nelly Burnichon and Yanli Ding and Dahia, {Patricia L.M.}",

note = "Funding Information: P.L.M.D. was supported by the National Institute of General Medical Sciences (NIGMS GM114102), CTSA-IIMS (National Institutes of Health (NIH)/National Center for Advancing Translational Sciences Grants UL1 TR001120 and UL1 TR002645), the Mays Cancer Center (NIH-National Cancer Institute (NCI) P30 CA54174), and Alex's Lemonade Stand Foundation for Childhood Cancer (with support from Northwest Mutual/Flashes of Hope) research grants. S.K.F. was supported by an NIGMS fellowship grant (F31GM131634) and, previously, by an NCI training grant (T32CA148724). The content is solely the responsibility of the authors and does not necessarily represent the official views of the NIH. The Central South University Xiangya School of Medicine, Changsha, Hunan, China, provided support to X.Z. D.B., T.D., and R.C.B. were supported by grants from the National Health and Medical Research Council (APP1108032), Hillcrest Foundation (Perpetual Trustees), and PheoPara Alliance. A.P.G.R. and N.B. were supported by the Institut National du Cancer and the Direction G{\'e}n{\'e}rale de l'Offre de Soins (PRT-K 2014, COMETE-TACTIC, INCa-DGOS_8663). L.F. was supported by the American Cancer Society Mentored Research Scholar Grant (MRSG-15-063-01-TBG). Publisher Copyright: {\textcopyright} 2020 The Author(s) 2020.",

year = "2021",

month = jan,

day = "1",

doi = "10.1210/clinem/dgaa741",

language = "English (US)",

volume = "106",

pages = "E350--E364",

journal = "Journal of Clinical Endocrinology and Metabolism",

issn = "0021-972X",

publisher = "The Endocrine Society",

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TY - JOUR

T1 - Genotype-phenotype features of germline variants of the TMEM127 pheochromocytoma susceptibility gene

T2 - A 10-year update

AU - Armaiz-Pena, Gustavo

AU - Flores, Shahida K.

AU - Cheng, Zi Ming

AU - Zhang, Xhingyu

AU - Esquivel, Emmanuel

AU - Poullard, Natalie

AU - Vaidyanathan, Anusha

AU - Liu, Qianqian

AU - Michalek, Joel

AU - Santillan-Gomez, Alfredo A.

AU - Liss, Michael

AU - Ahmadi, Sara

AU - Katselnik, Daniel

AU - Maldonado, Enrique

AU - Salgado, Sarimar Agosto

AU - Jimenez, Camilo

AU - Fishbein, Lauren

AU - Hamidi, Oksana

AU - Else, Tobias

AU - Lechan, Ron

AU - Tischler, Art S.

AU - Benn, Diana E.

AU - Dwight, Trisha

AU - Clifton-Bligh, Rory

AU - Sanso, Gabriela

AU - Barontini, Marta

AU - Vincent, Deepa

AU - Aronin, Neil

AU - Biondi, Bernadette

AU - Koops, Maureen

AU - Bowhay-Carnes, Elizabeth

AU - Gimenez-Roqueplo, Anne Paule

AU - Alvarez-Eslava, Andrea

AU - Bruder, Jan M.

AU - Kitano, Mio

AU - Burnichon, Nelly

AU - Ding, Yanli

AU - Dahia, Patricia L.M.

N1 - Funding Information: P.L.M.D. was supported by the National Institute of General Medical Sciences (NIGMS GM114102), CTSA-IIMS (National Institutes of Health (NIH)/National Center for Advancing Translational Sciences Grants UL1 TR001120 and UL1 TR002645), the Mays Cancer Center (NIH-National Cancer Institute (NCI) P30 CA54174), and Alex's Lemonade Stand Foundation for Childhood Cancer (with support from Northwest Mutual/Flashes of Hope) research grants. S.K.F. was supported by an NIGMS fellowship grant (F31GM131634) and, previously, by an NCI training grant (T32CA148724). The content is solely the responsibility of the authors and does not necessarily represent the official views of the NIH. The Central South University Xiangya School of Medicine, Changsha, Hunan, China, provided support to X.Z. D.B., T.D., and R.C.B. were supported by grants from the National Health and Medical Research Council (APP1108032), Hillcrest Foundation (Perpetual Trustees), and PheoPara Alliance. A.P.G.R. and N.B. were supported by the Institut National du Cancer and the Direction Générale de l'Offre de Soins (PRT-K 2014, COMETE-TACTIC, INCa-DGOS_8663). L.F. was supported by the American Cancer Society Mentored Research Scholar Grant (MRSG-15-063-01-TBG). Publisher Copyright: © 2020 The Author(s) 2020.

PY - 2021/1/1

Y1 - 2021/1/1

N2 - Purpose: This work aimed to evaluate genotype-phenotype associations in individuals carrying germline variants of transmembrane protein 127 gene (TMEM127), a poorly known gene that confers susceptibility to pheochromocytoma (PHEO) and paraganglioma (PGL). Design: Data were collected from a registry of probands with TMEM127 variants, published reports, and public databases. Main Outcome Analysis: Clinical, genetic, and functional associations were determined. Results: The cohort comprised 110 index patients (111 variants) with a mean age of 45 years (range, 21-84 years). Females were predominant (76 vs 34, P <. 001). Most patients had PHEO (n = 94; 85.5%), although PGL (n = 10; 9%) and renal cell carcinoma (RCC, n = 6; 5.4%) were also detected, either alone or in combination with PHEO. One-third of the cases had multiple tumors, and known family history was reported in 15.4%. Metastatic PHEO/PGL was rare (2.8%). Epinephrine alone, or combined with norepinephrine, accounted for 82% of the catecholamine profiles of PHEO/PGLs. Most variants (n = 63) occurred only once and 13 were recurrent (2-12 times). Although nontruncating variants were less frequent than truncating changes overall, they were predominant in non-PHEO clinical presentations (36% PHEO-only vs 69% other, P <. 001) and clustered disproportionately within transmembrane regions (P <. 01), underscoring the relevance of these domains for TMEM127 function. Integration of clinical and previous experimental data supported classification of variants into 4 groups based on mutation type, localization, and predicted disruption. Conclusions: Patients with TMEM127 variants often resemble sporadic nonmetastatic PHEOs. PGL and RCC may also co-occur, although their causal link requires further evaluation. We propose a new classification to predict variant pathogenicity and assist with carrier surveillance.

AB - Purpose: This work aimed to evaluate genotype-phenotype associations in individuals carrying germline variants of transmembrane protein 127 gene (TMEM127), a poorly known gene that confers susceptibility to pheochromocytoma (PHEO) and paraganglioma (PGL). Design: Data were collected from a registry of probands with TMEM127 variants, published reports, and public databases. Main Outcome Analysis: Clinical, genetic, and functional associations were determined. Results: The cohort comprised 110 index patients (111 variants) with a mean age of 45 years (range, 21-84 years). Females were predominant (76 vs 34, P <. 001). Most patients had PHEO (n = 94; 85.5%), although PGL (n = 10; 9%) and renal cell carcinoma (RCC, n = 6; 5.4%) were also detected, either alone or in combination with PHEO. One-third of the cases had multiple tumors, and known family history was reported in 15.4%. Metastatic PHEO/PGL was rare (2.8%). Epinephrine alone, or combined with norepinephrine, accounted for 82% of the catecholamine profiles of PHEO/PGLs. Most variants (n = 63) occurred only once and 13 were recurrent (2-12 times). Although nontruncating variants were less frequent than truncating changes overall, they were predominant in non-PHEO clinical presentations (36% PHEO-only vs 69% other, P <. 001) and clustered disproportionately within transmembrane regions (P <. 01), underscoring the relevance of these domains for TMEM127 function. Integration of clinical and previous experimental data supported classification of variants into 4 groups based on mutation type, localization, and predicted disruption. Conclusions: Patients with TMEM127 variants often resemble sporadic nonmetastatic PHEOs. PGL and RCC may also co-occur, although their causal link requires further evaluation. We propose a new classification to predict variant pathogenicity and assist with carrier surveillance.

KW - Genotype-phenotype association

KW - Paraganglioma

KW - Pheochromocytoma

KW - TMEM127

KW - Tumor suppressor gene

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Genotype-phenotype features of germline variants of the TMEM127 pheochromocytoma susceptibility gene: A 10-year update

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