65 YEARS OF THE DOUBLE HELIX Genetics informs precision practice in the diagnosis and management of pheochromocytoma

Hartmut P. Neumann; William F. Young; Tobias Krauss; Jean-Pierre Bayley; Francesca Schiavi; Giuseppe Opocher; Carsten C. Boedeker; Amit Tirosh; Frederic Castinetti; Juri Ruf; Dmitry Beltsevich; Martin Walz; Harald-Thomas Groeben; Ernst von Dobschuetz; Oliver Gimm; Nelson Wohllk; Marija Pfeifer; Delmar M. Lourenco; Mariola Peczkowska; Attila Patocs; Joanne Ngeow; Ozer Makay; Nalini S. Shah; Arthur Tischler; Helena Leijon; Gianmaria Pennelli; Karina Villar Gomez de las Heras; Thera P. Links; Birke Bausch; Charis Eng

doi:10.1530/ERC-18-0085

65 YEARS OF THE DOUBLE HELIX Genetics informs precision practice in the diagnosis and management of pheochromocytoma

Hartmut P. Neumann, William F. Young, Tobias Krauss, Jean-Pierre Bayley, Francesca Schiavi, Giuseppe Opocher, Carsten C. Boedeker, Amit Tirosh, Frederic Castinetti, Juri Ruf, Dmitry Beltsevich, Martin Walz, Harald-Thomas Groeben, Ernst von Dobschuetz, Oliver Gimm, Nelson Wohllk, Marija Pfeifer, Delmar M. Lourenco, Mariola Peczkowska, Attila PatocsJoanne Ngeow, Ozer Makay, Nalini S. Shah, Arthur Tischler, Helena Leijon, Gianmaria Pennelli, Karina Villar Gomez de las Heras, Thera P. Links, Birke Bausch^*, Charis Eng

^*Corresponding author for this work

Research output: Contribution to journal › Review article › peer-review

45 Citations (Scopus)

Abstract

Although the authors of the present review have contributed to genetic discoveries in the field of pheochromocytoma research, we can legitimately ask whether these advances have led to improvements in the diagnosis and management of patients with pheochromocytoma. The answer to this question is an emphatic Yes! In the field of molecular genetics, the well-established axiom that familial (genetic) pheochromocytoma represents 10% of all cases has been overturned, with >35% of cases now attributable to germline disease-causing mutations. Furthermore, genetic pheochromocytoma can now be grouped into five different clinical presentation types in the context of the ten known susceptibility genes for pheochromocytoma-associated syndromes. We now have the tools to diagnose patients with genetic pheochromocytoma, identify germline mutation carriers and to offer gene-informed medical management including enhanced surveillance and prevention. Clinically, we now treat an entire family of tumors of the paraganglia, with the exact phenotype varying by specific gene. In terms of detection and classification, simultaneous advances in biochemical detection and imaging localization have taken place, and the histopathology of the paraganglioma tumor family has been revised by immunohistochemical-genetic classification by gene-specific antibody immunohistochemistry. Treatment options have also been substantially enriched by the application of minimally invasive and adrenal-sparing surgery. Finally and most importantly, it is now widely recognized that patients with genetic pheochromocytoma/paraganglioma syndromes should be treated in specialized centers dedicated to the diagnosis, treatment and surveillance of this rare neoplasm.

Original language	English
Pages (from-to)	T201-T219
Number of pages	19
Journal	Endocrine-Related cancer
Volume	25
Issue number	8
DOIs	https://doi.org/10.1530/ERC-18-0085
Publication status	Published - Aug-2018

Keywords

brown adipose tissue
white adipose tissue
lipid metabolism
oxidative stress
ENDOCRINE NEOPLASIA TYPE-2
HIPPEL-LINDAU-DISEASE
TUMOR-SUPPRESSOR GENE
RENAL-CELL CARCINOMA
GERMLINE MUTATION CARRIERS
ADRENAL-SPARING SURGERY
SUCCINATE-DEHYDROGENASE
NEUROFIBROMATOSIS TYPE-1
RET PROTOONCOGENE
CASE SERIES

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65 YEARS OF THE DOUBLE HELIX: Genetics informs precision practice in the diagnosis and management of pheochromocytoma
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Neumann, H. P., Young, W. F., Krauss, T., Bayley, J-P., Schiavi, F., Opocher, G., Boedeker, C. C., Tirosh, A., Castinetti, F., Ruf, J., Beltsevich, D., Walz, M., Groeben, H-T., von Dobschuetz, E., Gimm, O., Wohllk, N., Pfeifer, M., Lourenco, D. M., Peczkowska, M., ... Eng, C. (2018). 65 YEARS OF THE DOUBLE HELIX Genetics informs precision practice in the diagnosis and management of pheochromocytoma. Endocrine-Related cancer, 25(8), T201-T219. https://doi.org/10.1530/ERC-18-0085

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title = "65 YEARS OF THE DOUBLE HELIX Genetics informs precision practice in the diagnosis and management of pheochromocytoma",

abstract = "Although the authors of the present review have contributed to genetic discoveries in the field of pheochromocytoma research, we can legitimately ask whether these advances have led to improvements in the diagnosis and management of patients with pheochromocytoma. The answer to this question is an emphatic Yes! In the field of molecular genetics, the well-established axiom that familial (genetic) pheochromocytoma represents 10% of all cases has been overturned, with >35% of cases now attributable to germline disease-causing mutations. Furthermore, genetic pheochromocytoma can now be grouped into five different clinical presentation types in the context of the ten known susceptibility genes for pheochromocytoma-associated syndromes. We now have the tools to diagnose patients with genetic pheochromocytoma, identify germline mutation carriers and to offer gene-informed medical management including enhanced surveillance and prevention. Clinically, we now treat an entire family of tumors of the paraganglia, with the exact phenotype varying by specific gene. In terms of detection and classification, simultaneous advances in biochemical detection and imaging localization have taken place, and the histopathology of the paraganglioma tumor family has been revised by immunohistochemical-genetic classification by gene-specific antibody immunohistochemistry. Treatment options have also been substantially enriched by the application of minimally invasive and adrenal-sparing surgery. Finally and most importantly, it is now widely recognized that patients with genetic pheochromocytoma/paraganglioma syndromes should be treated in specialized centers dedicated to the diagnosis, treatment and surveillance of this rare neoplasm.",

keywords = "brown adipose tissue, white adipose tissue, lipid metabolism, oxidative stress, ENDOCRINE NEOPLASIA TYPE-2, HIPPEL-LINDAU-DISEASE, TUMOR-SUPPRESSOR GENE, RENAL-CELL CARCINOMA, GERMLINE MUTATION CARRIERS, ADRENAL-SPARING SURGERY, SUCCINATE-DEHYDROGENASE, NEUROFIBROMATOSIS TYPE-1, RET PROTOONCOGENE, CASE SERIES",

author = "Neumann, {Hartmut P.} and Young, {William F.} and Tobias Krauss and Jean-Pierre Bayley and Francesca Schiavi and Giuseppe Opocher and Boedeker, {Carsten C.} and Amit Tirosh and Frederic Castinetti and Juri Ruf and Dmitry Beltsevich and Martin Walz and Harald-Thomas Groeben and {von Dobschuetz}, Ernst and Oliver Gimm and Nelson Wohllk and Marija Pfeifer and Lourenco, {Delmar M.} and Mariola Peczkowska and Attila Patocs and Joanne Ngeow and Ozer Makay and Shah, {Nalini S.} and Arthur Tischler and Helena Leijon and Gianmaria Pennelli and {Villar Gomez de las Heras}, Karina and Links, {Thera P.} and Birke Bausch and Charis Eng",

year = "2018",

month = aug,

doi = "10.1530/ERC-18-0085",

language = "English",

volume = "25",

pages = "T201--T219",

journal = "Endocrine-Related cancer",

issn = "1351-0088",

publisher = "BIOSCIENTIFICA LTD",

number = "8",

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Neumann, HP, Young, WF, Krauss, T, Bayley, J-P, Schiavi, F, Opocher, G, Boedeker, CC, Tirosh, A, Castinetti, F, Ruf, J, Beltsevich, D, Walz, M, Groeben, H-T, von Dobschuetz, E, Gimm, O, Wohllk, N, Pfeifer, M, Lourenco, DM, Peczkowska, M, Patocs, A, Ngeow, J, Makay, O, Shah, NS, Tischler, A, Leijon, H, Pennelli, G, Villar Gomez de las Heras, K, Links, TP, Bausch, B & Eng, C 2018, '65 YEARS OF THE DOUBLE HELIX Genetics informs precision practice in the diagnosis and management of pheochromocytoma', Endocrine-Related cancer, vol. 25, no. 8, pp. T201-T219. https://doi.org/10.1530/ERC-18-0085

TY - JOUR

T1 - 65 YEARS OF THE DOUBLE HELIX Genetics informs precision practice in the diagnosis and management of pheochromocytoma

AU - Neumann, Hartmut P.

AU - Young, William F.

AU - Krauss, Tobias

AU - Bayley, Jean-Pierre

AU - Schiavi, Francesca

AU - Opocher, Giuseppe

AU - Boedeker, Carsten C.

AU - Tirosh, Amit

AU - Castinetti, Frederic

AU - Ruf, Juri

AU - Beltsevich, Dmitry

AU - Walz, Martin

AU - Groeben, Harald-Thomas

AU - von Dobschuetz, Ernst

AU - Gimm, Oliver

AU - Wohllk, Nelson

AU - Pfeifer, Marija

AU - Lourenco, Delmar M.

AU - Peczkowska, Mariola

AU - Patocs, Attila

AU - Ngeow, Joanne

AU - Makay, Ozer

AU - Shah, Nalini S.

AU - Tischler, Arthur

AU - Leijon, Helena

AU - Pennelli, Gianmaria

AU - Villar Gomez de las Heras, Karina

AU - Links, Thera P.

AU - Bausch, Birke

AU - Eng, Charis

PY - 2018/8

Y1 - 2018/8

N2 - Although the authors of the present review have contributed to genetic discoveries in the field of pheochromocytoma research, we can legitimately ask whether these advances have led to improvements in the diagnosis and management of patients with pheochromocytoma. The answer to this question is an emphatic Yes! In the field of molecular genetics, the well-established axiom that familial (genetic) pheochromocytoma represents 10% of all cases has been overturned, with >35% of cases now attributable to germline disease-causing mutations. Furthermore, genetic pheochromocytoma can now be grouped into five different clinical presentation types in the context of the ten known susceptibility genes for pheochromocytoma-associated syndromes. We now have the tools to diagnose patients with genetic pheochromocytoma, identify germline mutation carriers and to offer gene-informed medical management including enhanced surveillance and prevention. Clinically, we now treat an entire family of tumors of the paraganglia, with the exact phenotype varying by specific gene. In terms of detection and classification, simultaneous advances in biochemical detection and imaging localization have taken place, and the histopathology of the paraganglioma tumor family has been revised by immunohistochemical-genetic classification by gene-specific antibody immunohistochemistry. Treatment options have also been substantially enriched by the application of minimally invasive and adrenal-sparing surgery. Finally and most importantly, it is now widely recognized that patients with genetic pheochromocytoma/paraganglioma syndromes should be treated in specialized centers dedicated to the diagnosis, treatment and surveillance of this rare neoplasm.

AB - Although the authors of the present review have contributed to genetic discoveries in the field of pheochromocytoma research, we can legitimately ask whether these advances have led to improvements in the diagnosis and management of patients with pheochromocytoma. The answer to this question is an emphatic Yes! In the field of molecular genetics, the well-established axiom that familial (genetic) pheochromocytoma represents 10% of all cases has been overturned, with >35% of cases now attributable to germline disease-causing mutations. Furthermore, genetic pheochromocytoma can now be grouped into five different clinical presentation types in the context of the ten known susceptibility genes for pheochromocytoma-associated syndromes. We now have the tools to diagnose patients with genetic pheochromocytoma, identify germline mutation carriers and to offer gene-informed medical management including enhanced surveillance and prevention. Clinically, we now treat an entire family of tumors of the paraganglia, with the exact phenotype varying by specific gene. In terms of detection and classification, simultaneous advances in biochemical detection and imaging localization have taken place, and the histopathology of the paraganglioma tumor family has been revised by immunohistochemical-genetic classification by gene-specific antibody immunohistochemistry. Treatment options have also been substantially enriched by the application of minimally invasive and adrenal-sparing surgery. Finally and most importantly, it is now widely recognized that patients with genetic pheochromocytoma/paraganglioma syndromes should be treated in specialized centers dedicated to the diagnosis, treatment and surveillance of this rare neoplasm.

KW - brown adipose tissue

KW - white adipose tissue

KW - lipid metabolism

KW - oxidative stress

KW - ENDOCRINE NEOPLASIA TYPE-2

KW - HIPPEL-LINDAU-DISEASE

KW - TUMOR-SUPPRESSOR GENE

KW - RENAL-CELL CARCINOMA

KW - GERMLINE MUTATION CARRIERS

KW - ADRENAL-SPARING SURGERY

KW - SUCCINATE-DEHYDROGENASE

KW - NEUROFIBROMATOSIS TYPE-1

KW - RET PROTOONCOGENE

KW - CASE SERIES

U2 - 10.1530/ERC-18-0085

DO - 10.1530/ERC-18-0085

M3 - Review article

SN - 1351-0088

VL - 25

SP - T201-T219

JO - Endocrine-Related cancer

JF - Endocrine-Related cancer

IS - 8

ER -