Di-genic inheritance of germline POLE and PMS2 pathogenic variants causes a unique condition associated with pediatric cancer predisposition

Orli Michaeli; Hagay Ladany; Ayelet Erez; Shay Ben Shachar; Shai Izraeli; Gabriel Lidzbarsky; Lina Basel-Salmon; Saskia Biskup; Yosef E. Maruvka; Helen Toledano; Yael Goldberg

doi:10.1111/cge.14106

Di-genic inheritance of germline POLE and PMS2 pathogenic variants causes a unique condition associated with pediatric cancer predisposition

Orli Michaeli, Hagay Ladany, Ayelet Erez, Shay Ben Shachar, Shai Izraeli, Gabriel Lidzbarsky, Lina Basel-Salmon, Saskia Biskup, Yosef E. Maruvka, Helen Toledano, Yael Goldberg

Tel Aviv University, Weizmann Institute of Science, Technion - Israel Institute of Technology

Research output: Contribution to journal › Article › peer-review

Abstract

Polymerase proofreading-associated polyposis (PPAP) and Lynch syndrome, caused by mutated POLE and mismatch repair (MMR) genes, respectively, are associated with adult-onset cancer. PPAP and MMR-deficient tumors are both hypermutated, and each has a unique mutational signature. We describe a 4.5-year-old boy with multiple café au lait spots who presented with metastatic Sonic Hedgehog-activated medulloblastoma, with partial response to intensive chemotherapy and immunotherapy. The tumor showed microsatellite stability, loss of PMS2 nuclear expression, and an exceptionally high tumor mutational burden of 276 Mut/Mb. Germline molecular analysis revealed an inherited heterozygous pathogenic POLE variant and a de novo heterozygous PMS2 pathogenic variant. The tumor featured the MMR, POLE, and POLE+MMR mutational signatures. This is the first description of a di-genic condition, which we named “POL-LYNCH syndrome,” manifested by an aggressive ultra-mutant pediatric medulloblastoma with a unique genomic signature.

Original language	English
Pages (from-to)	442-447
Number of pages	6
Journal	Clinical Genetics
Volume	101
Issue number	4
DOIs	https://doi.org/10.1111/cge.14106
State	Published - Apr 2022

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

LYNCH
PMS2
POLE
di-genic
genomic signature
medulloblastoma

All Science Journal Classification (ASJC) codes

Genetics
Genetics(clinical)

Access to Document

10.1111/cge.14106

Cite this

Michaeli, O., Ladany, H., Erez, A., Ben Shachar, S., Izraeli, S., Lidzbarsky, G., Basel-Salmon, L., Biskup, S., Maruvka, Y. E., Toledano, H., & Goldberg, Y. (2022). Di-genic inheritance of germline POLE and PMS2 pathogenic variants causes a unique condition associated with pediatric cancer predisposition. Clinical Genetics, 101(4), 442-447. https://doi.org/10.1111/cge.14106

@article{50b791c4e9554d42a065f20632f94a6a,

title = "Di-genic inheritance of germline POLE and PMS2 pathogenic variants causes a unique condition associated with pediatric cancer predisposition",

abstract = "Polymerase proofreading-associated polyposis (PPAP) and Lynch syndrome, caused by mutated POLE and mismatch repair (MMR) genes, respectively, are associated with adult-onset cancer. PPAP and MMR-deficient tumors are both hypermutated, and each has a unique mutational signature. We describe a 4.5-year-old boy with multiple caf{\'e} au lait spots who presented with metastatic Sonic Hedgehog-activated medulloblastoma, with partial response to intensive chemotherapy and immunotherapy. The tumor showed microsatellite stability, loss of PMS2 nuclear expression, and an exceptionally high tumor mutational burden of 276 Mut/Mb. Germline molecular analysis revealed an inherited heterozygous pathogenic POLE variant and a de novo heterozygous PMS2 pathogenic variant. The tumor featured the MMR, POLE, and POLE+MMR mutational signatures. This is the first description of a di-genic condition, which we named “POL-LYNCH syndrome,” manifested by an aggressive ultra-mutant pediatric medulloblastoma with a unique genomic signature.",

keywords = "LYNCH, PMS2, POLE, di-genic, genomic signature, medulloblastoma",

author = "Orli Michaeli and Hagay Ladany and Ayelet Erez and \{Ben Shachar\}, Shay and Shai Izraeli and Gabriel Lidzbarsky and Lina Basel-Salmon and Saskia Biskup and Maruvka, \{Yosef E.\} and Helen Toledano and Yael Goldberg",

note = "Publisher Copyright: {\textcopyright} 2021 John Wiley \& Sons A/S. Published by John Wiley \& Sons Ltd",

year = "2022",

month = apr,

doi = "10.1111/cge.14106",

language = "الإنجليزيّة",

volume = "101",

pages = "442--447",

journal = "Clinical Genetics",

issn = "0009-9163",

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Michaeli, O, Ladany, H, Erez, A, Ben Shachar, S, Izraeli, S, Lidzbarsky, G, Basel-Salmon, L, Biskup, S, Maruvka, YE, Toledano, H & Goldberg, Y 2022, 'Di-genic inheritance of germline POLE and PMS2 pathogenic variants causes a unique condition associated with pediatric cancer predisposition', Clinical Genetics, vol. 101, no. 4, pp. 442-447. https://doi.org/10.1111/cge.14106

TY - JOUR

T1 - Di-genic inheritance of germline POLE and PMS2 pathogenic variants causes a unique condition associated with pediatric cancer predisposition

AU - Michaeli, Orli

AU - Ladany, Hagay

AU - Erez, Ayelet

AU - Ben Shachar, Shay

AU - Izraeli, Shai

AU - Lidzbarsky, Gabriel

AU - Basel-Salmon, Lina

AU - Biskup, Saskia

AU - Maruvka, Yosef E.

AU - Toledano, Helen

AU - Goldberg, Yael

PY - 2022/4

Y1 - 2022/4

N2 - Polymerase proofreading-associated polyposis (PPAP) and Lynch syndrome, caused by mutated POLE and mismatch repair (MMR) genes, respectively, are associated with adult-onset cancer. PPAP and MMR-deficient tumors are both hypermutated, and each has a unique mutational signature. We describe a 4.5-year-old boy with multiple café au lait spots who presented with metastatic Sonic Hedgehog-activated medulloblastoma, with partial response to intensive chemotherapy and immunotherapy. The tumor showed microsatellite stability, loss of PMS2 nuclear expression, and an exceptionally high tumor mutational burden of 276 Mut/Mb. Germline molecular analysis revealed an inherited heterozygous pathogenic POLE variant and a de novo heterozygous PMS2 pathogenic variant. The tumor featured the MMR, POLE, and POLE+MMR mutational signatures. This is the first description of a di-genic condition, which we named “POL-LYNCH syndrome,” manifested by an aggressive ultra-mutant pediatric medulloblastoma with a unique genomic signature.

AB - Polymerase proofreading-associated polyposis (PPAP) and Lynch syndrome, caused by mutated POLE and mismatch repair (MMR) genes, respectively, are associated with adult-onset cancer. PPAP and MMR-deficient tumors are both hypermutated, and each has a unique mutational signature. We describe a 4.5-year-old boy with multiple café au lait spots who presented with metastatic Sonic Hedgehog-activated medulloblastoma, with partial response to intensive chemotherapy and immunotherapy. The tumor showed microsatellite stability, loss of PMS2 nuclear expression, and an exceptionally high tumor mutational burden of 276 Mut/Mb. Germline molecular analysis revealed an inherited heterozygous pathogenic POLE variant and a de novo heterozygous PMS2 pathogenic variant. The tumor featured the MMR, POLE, and POLE+MMR mutational signatures. This is the first description of a di-genic condition, which we named “POL-LYNCH syndrome,” manifested by an aggressive ultra-mutant pediatric medulloblastoma with a unique genomic signature.

KW - LYNCH

KW - PMS2

KW - POLE

KW - di-genic

KW - genomic signature

KW - medulloblastoma

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U2 - 10.1111/cge.14106

DO - 10.1111/cge.14106

M3 - مقالة

C2 - 34967012

SN - 0009-9163

VL - 101

SP - 442

EP - 447

JO - Clinical Genetics

JF - Clinical Genetics

IS - 4

ER -

Di-genic inheritance of germline POLE and PMS2 pathogenic variants causes a unique condition associated with pediatric cancer predisposition

Abstract

UN SDGs

Keywords

All Science Journal Classification (ASJC) codes

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