Epidemiology, biology and therapy of Merkel cell carcinoma: conclusions from the EU project IMMOMEC

Juergen C. Becker; Andreas Stang; Axel zur Hausen; Nicole Fischer; James A. DeCaprio; Richard W. Tothill; Rikke Lyngaa; Ulla Kring Hansen; Cathrin Ritter; Paul Nghiem; Christopher K. Bichakjian; Selma Ugurel; David Schrama

doi:10.1007/s00262-017-2099-3

Epidemiology, biology and therapy of Merkel cell carcinoma: conclusions from the EU project IMMOMEC

Juergen C. Becker^*, Andreas Stang, Axel zur Hausen, Nicole Fischer, James A. DeCaprio, Richard W. Tothill, Rikke Lyngaa, Ulla Kring Hansen, Cathrin Ritter, Paul Nghiem, Christopher K. Bichakjian, Selma Ugurel, David Schrama

^*Corresponding author for this work

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

Abstract

Merkel cell carcinoma (MCC) is a highly aggressive, often lethal neuroendocrine cancer. Its carcinogenesis may be either caused by the clonal integration of the Merkel cell polyomavirus into the host genome or by UV-induced mutations. Notably, virally-encoded oncoproteins and UV-induced mutations affect comparable signaling pathways such as RB restriction of cell cycle progression or p53 inactivation. Despite its low incidence, MCC recently received much attention based on its exquisite immunogenicity and the resulting major success of immune modulating therapies. Here, we summarize current knowledge on epidemiology, biology and therapy of MCC as conclusion of the project 'Immune Modulating strategies for treatment of Merkel Cell Carcinoma', which was funded over a 5-year period by the European Commission to investigate innovative immunotherapies for MCC.

Original language	English
Pages (from-to)	341-351
Number of pages	11
Journal	Cancer Immunology Immunotherapy
Volume	67
Issue number	3
DOIs	https://doi.org/10.1007/s00262-017-2099-3
Publication status	Published - 1 Mar 2018

Keywords

Merkel cell carcinoma
Epidemiology
Cell of origin
Merkel cell polyomavirus
Immunotherapy
IMMOMEC
SMALL T-ANTIGEN
DOWN-REGULATION
POLYOMAVIRUS
EXPRESSION
RECURRENCE
GROWTH
PROLIFERATION
INHIBITION
PREVALENT
SURVIVAL

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10.1007/s00262-017-2099-3

Cite this

Becker, J. C., Stang, A., zur Hausen, A., Fischer, N., DeCaprio, J. A., Tothill, R. W., Lyngaa, R., Hansen, U. K., Ritter, C., Nghiem, P., Bichakjian, C. K., Ugurel, S., & Schrama, D. (2018). Epidemiology, biology and therapy of Merkel cell carcinoma: conclusions from the EU project IMMOMEC. Cancer Immunology Immunotherapy, 67(3), 341-351. https://doi.org/10.1007/s00262-017-2099-3

@article{a51c5601d5844c588c55d27c10d87099,

title = "Epidemiology, biology and therapy of Merkel cell carcinoma: conclusions from the EU project IMMOMEC",

abstract = "Merkel cell carcinoma (MCC) is a highly aggressive, often lethal neuroendocrine cancer. Its carcinogenesis may be either caused by the clonal integration of the Merkel cell polyomavirus into the host genome or by UV-induced mutations. Notably, virally-encoded oncoproteins and UV-induced mutations affect comparable signaling pathways such as RB restriction of cell cycle progression or p53 inactivation. Despite its low incidence, MCC recently received much attention based on its exquisite immunogenicity and the resulting major success of immune modulating therapies. Here, we summarize current knowledge on epidemiology, biology and therapy of MCC as conclusion of the project 'Immune Modulating strategies for treatment of Merkel Cell Carcinoma', which was funded over a 5-year period by the European Commission to investigate innovative immunotherapies for MCC.",

keywords = "Merkel cell carcinoma, Epidemiology, Cell of origin, Merkel cell polyomavirus, Immunotherapy, IMMOMEC, SMALL T-ANTIGEN, DOWN-REGULATION, POLYOMAVIRUS, EXPRESSION, RECURRENCE, GROWTH, PROLIFERATION, INHIBITION, PREVALENT, SURVIVAL",

author = "Becker, {Juergen C.} and Andreas Stang and {zur Hausen}, Axel and Nicole Fischer and DeCaprio, {James A.} and Tothill, {Richard W.} and Rikke Lyngaa and Hansen, {Ulla Kring} and Cathrin Ritter and Paul Nghiem and Bichakjian, {Christopher K.} and Selma Ugurel and David Schrama",

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doi = "10.1007/s00262-017-2099-3",

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Becker, JC, Stang, A, zur Hausen, A, Fischer, N, DeCaprio, JA, Tothill, RW, Lyngaa, R, Hansen, UK, Ritter, C, Nghiem, P, Bichakjian, CK, Ugurel, S & Schrama, D 2018, 'Epidemiology, biology and therapy of Merkel cell carcinoma: conclusions from the EU project IMMOMEC', Cancer Immunology Immunotherapy, vol. 67, no. 3, pp. 341-351. https://doi.org/10.1007/s00262-017-2099-3

TY - JOUR

T1 - Epidemiology, biology and therapy of Merkel cell carcinoma

T2 - conclusions from the EU project IMMOMEC

AU - Becker, Juergen C.

AU - Stang, Andreas

AU - zur Hausen, Axel

AU - Fischer, Nicole

AU - DeCaprio, James A.

AU - Tothill, Richard W.

AU - Lyngaa, Rikke

AU - Hansen, Ulla Kring

AU - Ritter, Cathrin

AU - Nghiem, Paul

AU - Bichakjian, Christopher K.

AU - Ugurel, Selma

AU - Schrama, David

PY - 2018/3/1

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N2 - Merkel cell carcinoma (MCC) is a highly aggressive, often lethal neuroendocrine cancer. Its carcinogenesis may be either caused by the clonal integration of the Merkel cell polyomavirus into the host genome or by UV-induced mutations. Notably, virally-encoded oncoproteins and UV-induced mutations affect comparable signaling pathways such as RB restriction of cell cycle progression or p53 inactivation. Despite its low incidence, MCC recently received much attention based on its exquisite immunogenicity and the resulting major success of immune modulating therapies. Here, we summarize current knowledge on epidemiology, biology and therapy of MCC as conclusion of the project 'Immune Modulating strategies for treatment of Merkel Cell Carcinoma', which was funded over a 5-year period by the European Commission to investigate innovative immunotherapies for MCC.

AB - Merkel cell carcinoma (MCC) is a highly aggressive, often lethal neuroendocrine cancer. Its carcinogenesis may be either caused by the clonal integration of the Merkel cell polyomavirus into the host genome or by UV-induced mutations. Notably, virally-encoded oncoproteins and UV-induced mutations affect comparable signaling pathways such as RB restriction of cell cycle progression or p53 inactivation. Despite its low incidence, MCC recently received much attention based on its exquisite immunogenicity and the resulting major success of immune modulating therapies. Here, we summarize current knowledge on epidemiology, biology and therapy of MCC as conclusion of the project 'Immune Modulating strategies for treatment of Merkel Cell Carcinoma', which was funded over a 5-year period by the European Commission to investigate innovative immunotherapies for MCC.

KW - Merkel cell carcinoma

KW - Epidemiology

KW - Cell of origin

KW - Merkel cell polyomavirus

KW - Immunotherapy

KW - IMMOMEC

KW - SMALL T-ANTIGEN

KW - DOWN-REGULATION

KW - POLYOMAVIRUS

KW - EXPRESSION

KW - RECURRENCE

KW - GROWTH

KW - PROLIFERATION

KW - INHIBITION

KW - PREVALENT

KW - SURVIVAL

U2 - 10.1007/s00262-017-2099-3

DO - 10.1007/s00262-017-2099-3

M3 - (Systematic) Review article

C2 - 29188306

SN - 0340-7004

VL - 67

SP - 341

EP - 351

JO - Cancer Immunology Immunotherapy

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ER -