Classification of PRSS1 variants responsible for chronic pancreatitis: An expert perspective from the Franco-Chinese GREPAN Study Group

France

doi:10.1016/j.pan.2023.04.004

Classification of PRSS1 variants responsible for chronic pancreatitis: An expert perspective from the Franco-Chinese GREPAN Study Group

France

Université de Bretagne Occidentale
CHU de Brest
Shanghai Changhai Hospital
Shanghai Institute of Pancreatic Diseases
Nanjing University
Department of Hepatobiliopancreatic Surgery
CH Cornouaille
CHU Dupuytren
CHU de Toulouse
Hôpital Tenon
CHU Nantes
CH Cholet
Hospital of Saint-Etienne
CHI d'Aulnay-sous-Bois
Avignon Hospital
Le Havre Hospital
Hôpital de la Croix-Rousse
HIA Clermont-Tonnerre
CHU de Clermont-Ferrand
CH Saint Brieuc
CHU de Reims
Sorbonne Université
CHR d'Orléans
CHRU Strasbourg
Hôpital Antoine Béclère
Hôpital Robert Debré, CHU de Reims
Hôpital Louis Mourier
CH Cahors
CH Chartres
Université de Bourgogne
CHU de Grenoble
Hôpital Pasteur Colmar
CH Saint-Malo
The First Affiliated Hospital of Xi’an Jiaotong University
Groupe hospitalier Pellegrin
Assistance publique - Hôpitaux de Marseille
CH Blois
CHU de Nice
CH des Escartons
Hôpital Privé Jean Mermoz
Centre Hospitalier de Mulhouse
Institut Paoli Calmettes
CHU de Rennes
CH Bretagne Atlantique
CH Dax-Côte d'Argent
GH Diaconesses
CHI Villeneuve Saint Georges
Hospices civils de Lyon
CH Chartres
Hôpital d'instruction des armées Percy
Université de Franche-Comté
Clinique Sainte Barbe
CHU de Poitiers
CHU Amiens Picardie
CHU Hôpitaux de Rouen
Centre Hospitalier Régional Universitaire de Tours
Université d'Angers
Université Paris Cité
Hôpital Édouard Herriot
Hôpital Saint-Joseph
CHI de Créteil
Clinique Charcot
Hôpital Dreux
University Hospital
CH Melun
CHU Montpellier
CH Bastia
the Second Affiliated Hospital of Wenzhou Medical University
Chinese Academy of Medical Sciences
Peking University
Shanghai Jiao Tong University
Southern Medical University
Shengjing Hospital
Chinese PLA No.928 Hospital
Cancer Center of the Fifth Affiliated Hospital of Sun Yat-sen University
First Affiliated Hospital of Sun Yat sen University
Ningxia Medical University
Shenzhen University
Sichuan University
Fujian Medical University
Yangzhou University
The First Affiliated Hospital with Nanjing Medical University
The First Affiliated Hospital of Wenzhou Medical University
The First Affiliated Hospital of Harbin Medical University
Heilongjiang Provincial Hospital
Qingdao University
Guangdong Academy of Medical Sciences
Fudan University
Hebei Medical University
Guizhou Provincial People's Hospital
Shanxi Medical University
The People's Hospital of Longhua
Binzhou Medical University
Shenyang General Hospital of PLA
970 Hospital of PLA
Shenzhen People's Hospital
Xijing Hospital
Hangzhou First People's Hospital
Wuhan Union Hospital
Guangdong Provincial Hospital of Traditional Chinese Medicine
Nanfang Hospital
Shaanxi University of Chinese Medicine
Xiamen Humanity Hospital
Anhui Medical University
Qinghai Provincial People's Hospital
Lanzhou University
Cardiff University

科研成果: 期刊稿件 › 文章 › 同行评审

11 引用（Scopus）

摘要

Background: PRSS1 was the first reported chronic pancreatitis (CP) gene. The existence of both gain-of-function (GoF) and gain-of-proteotoxicity (GoP) pathological PRSS1 variants, together with the fact that PRSS1 variants have been identified in CP subtypes spanning the range from monogenic to multifactorial, has made the classification of PRSS1 variants very challenging. Methods: All currently reported PRSS1 variants (derived primarily from two databases) were manually reviewed with respect to their clinical genetics, functional analysis and population allele frequency. They were classified by variant type and pathological mechanism within the framework of our recently proposed ACMG/AMP guidelines-based seven-category system. Results: The total number of distinct germline PRSS1 variants included for analysis was 100, comprising 3 copy number variants (CNVs), 12 5′ and 3′ variants, 19 intronic variants, 5 nonsense variants, 1 frameshift deletion variant, 6 synonymous variants, 1 in-frame duplication, 3 gene conversions and 50 missense variants. Based upon a combination of clinical genetic and functional analysis, population data and in silico analysis, we classified 26 variants (all 3 CNVs, the in-frame duplication, all 3 gene conversions and 19 missense) as “pathogenic”, 3 variants (missense) as “likely pathogenic”, 5 variants (four missense and one promoter) as “predisposing”, 13 variants (all missense) as “unknown significance”, 2 variants (missense) as “likely benign”, and all remaining 51 variants as “benign”. Conclusions: We describe an expert classification of the 100 PRSS1 variants reported to date. The results have immediate implications for reclassifying many ClinVar-registered PRSS1 variants as well as providing optimal guidelines/standards for reporting PRSS1 variants.

源语言	英语
页（从-至）	491-506
页数	16
期刊	Pancreatology
卷	23
期	5
DOI	https://doi.org/10.1016/j.pan.2023.04.004
出版状态	已出版 - 8月 2023
已对外发布	是

联合国可持续发展目标

此成果有助于实现下列可持续发展目标：

可持续发展目标 3 良好健康与福祉

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10.1016/j.pan.2023.04.004

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引用此

@article{34ed6c02d64c45e694f7971eaf988253,

title = "Classification of PRSS1 variants responsible for chronic pancreatitis: An expert perspective from the Franco-Chinese GREPAN Study Group",

abstract = "Background: PRSS1 was the first reported chronic pancreatitis (CP) gene. The existence of both gain-of-function (GoF) and gain-of-proteotoxicity (GoP) pathological PRSS1 variants, together with the fact that PRSS1 variants have been identified in CP subtypes spanning the range from monogenic to multifactorial, has made the classification of PRSS1 variants very challenging. Methods: All currently reported PRSS1 variants (derived primarily from two databases) were manually reviewed with respect to their clinical genetics, functional analysis and population allele frequency. They were classified by variant type and pathological mechanism within the framework of our recently proposed ACMG/AMP guidelines-based seven-category system. Results: The total number of distinct germline PRSS1 variants included for analysis was 100, comprising 3 copy number variants (CNVs), 12 5′ and 3′ variants, 19 intronic variants, 5 nonsense variants, 1 frameshift deletion variant, 6 synonymous variants, 1 in-frame duplication, 3 gene conversions and 50 missense variants. Based upon a combination of clinical genetic and functional analysis, population data and in silico analysis, we classified 26 variants (all 3 CNVs, the in-frame duplication, all 3 gene conversions and 19 missense) as “pathogenic”, 3 variants (missense) as “likely pathogenic”, 5 variants (four missense and one promoter) as “predisposing”, 13 variants (all missense) as “unknown significance”, 2 variants (missense) as “likely benign”, and all remaining 51 variants as “benign”. Conclusions: We describe an expert classification of the 100 PRSS1 variants reported to date. The results have immediate implications for reclassifying many ClinVar-registered PRSS1 variants as well as providing optimal guidelines/standards for reporting PRSS1 variants.",

keywords = "Chronic pancreatitis, Genetic predisposition to disease, PRSS1 gene, Trypsinogen/trypsin, Variant classification",

author = "France and Emmanuelle Masson and Zou, \{Wen Bin\} and Na Pu and Vinciane Rebours and Emmanuelle G{\'e}nin and Hao Wu and Lin, \{Jin Huan\} and Wang, \{Yuan Chen\} and Amandine Abrantes and \{Aguilera Munoz\}, Lina and J{\'e}r{\'e}mie Albouys and Laurent Alric and Xavier Amiot and Isabelle Archambeaud and Sol{\`e}ne Audiau and Laetitia Bastide and Julien Baudon and Guy Bellaiche and Serge Bellon and Val{\'e}rie Bertrand and Karine Bideau and Kareen Billiemaz and Claire Billioud and Sabine Bonnefoy and Corinne Borderon and Barbara Bournet and Estelle Breton and Mathias Brugel and Louis Buscail and Guillaume Cadiot and Marine Camus and Xavier Causse and Patrick Chamouard and Ulriikka Chaput and Franck Cholet and Ciocan, \{Dragos Marius\} and Christine Clavel and Benoit Coffin and Laura Coimet-Berger and Isabelle Creveaux and Adrian Culetto and Oussama Daboussi and \{De Mestier\}, Louis and Thibault Degand and Christelle D'Engremont and Bernard Denis and Sol{\`e}ne Dermine and Romain Desgrippes and \{Drouet D'Aubigny\}, Augustin and Zheng Wang",

note = "Publisher Copyright: {\textcopyright} 2023 IAP and EPC",

year = "2023",

month = aug,

doi = "10.1016/j.pan.2023.04.004",

language = "英语",

volume = "23",

pages = "491--506",

journal = "Pancreatology",

issn = "1424-3903",

publisher = "Elsevier B.V.",

number = "5",

}

TY - JOUR

T1 - Classification of PRSS1 variants responsible for chronic pancreatitis

T2 - An expert perspective from the Franco-Chinese GREPAN Study Group

AU - France

AU - Masson, Emmanuelle

AU - Zou, Wen Bin

AU - Pu, Na

AU - Rebours, Vinciane

AU - Génin, Emmanuelle

AU - Wu, Hao

AU - Lin, Jin Huan

AU - Wang, Yuan Chen

AU - Abrantes, Amandine

AU - Aguilera Munoz, Lina

AU - Albouys, Jérémie

AU - Alric, Laurent

AU - Amiot, Xavier

AU - Archambeaud, Isabelle

AU - Audiau, Solène

AU - Bastide, Laetitia

AU - Baudon, Julien

AU - Bellaiche, Guy

AU - Bellon, Serge

AU - Bertrand, Valérie

AU - Bideau, Karine

AU - Billiemaz, Kareen

AU - Billioud, Claire

AU - Bonnefoy, Sabine

AU - Borderon, Corinne

AU - Bournet, Barbara

AU - Breton, Estelle

AU - Brugel, Mathias

AU - Buscail, Louis

AU - Cadiot, Guillaume

AU - Camus, Marine

AU - Causse, Xavier

AU - Chamouard, Patrick

AU - Chaput, Ulriikka

AU - Cholet, Franck

AU - Ciocan, Dragos Marius

AU - Clavel, Christine

AU - Coffin, Benoit

AU - Coimet-Berger, Laura

AU - Creveaux, Isabelle

AU - Culetto, Adrian

AU - Daboussi, Oussama

AU - De Mestier, Louis

AU - Degand, Thibault

AU - D'Engremont, Christelle

AU - Denis, Bernard

AU - Dermine, Solène

AU - Desgrippes, Romain

AU - Drouet D'Aubigny, Augustin

AU - Wang, Zheng

PY - 2023/8

Y1 - 2023/8

N2 - Background: PRSS1 was the first reported chronic pancreatitis (CP) gene. The existence of both gain-of-function (GoF) and gain-of-proteotoxicity (GoP) pathological PRSS1 variants, together with the fact that PRSS1 variants have been identified in CP subtypes spanning the range from monogenic to multifactorial, has made the classification of PRSS1 variants very challenging. Methods: All currently reported PRSS1 variants (derived primarily from two databases) were manually reviewed with respect to their clinical genetics, functional analysis and population allele frequency. They were classified by variant type and pathological mechanism within the framework of our recently proposed ACMG/AMP guidelines-based seven-category system. Results: The total number of distinct germline PRSS1 variants included for analysis was 100, comprising 3 copy number variants (CNVs), 12 5′ and 3′ variants, 19 intronic variants, 5 nonsense variants, 1 frameshift deletion variant, 6 synonymous variants, 1 in-frame duplication, 3 gene conversions and 50 missense variants. Based upon a combination of clinical genetic and functional analysis, population data and in silico analysis, we classified 26 variants (all 3 CNVs, the in-frame duplication, all 3 gene conversions and 19 missense) as “pathogenic”, 3 variants (missense) as “likely pathogenic”, 5 variants (four missense and one promoter) as “predisposing”, 13 variants (all missense) as “unknown significance”, 2 variants (missense) as “likely benign”, and all remaining 51 variants as “benign”. Conclusions: We describe an expert classification of the 100 PRSS1 variants reported to date. The results have immediate implications for reclassifying many ClinVar-registered PRSS1 variants as well as providing optimal guidelines/standards for reporting PRSS1 variants.

AB - Background: PRSS1 was the first reported chronic pancreatitis (CP) gene. The existence of both gain-of-function (GoF) and gain-of-proteotoxicity (GoP) pathological PRSS1 variants, together with the fact that PRSS1 variants have been identified in CP subtypes spanning the range from monogenic to multifactorial, has made the classification of PRSS1 variants very challenging. Methods: All currently reported PRSS1 variants (derived primarily from two databases) were manually reviewed with respect to their clinical genetics, functional analysis and population allele frequency. They were classified by variant type and pathological mechanism within the framework of our recently proposed ACMG/AMP guidelines-based seven-category system. Results: The total number of distinct germline PRSS1 variants included for analysis was 100, comprising 3 copy number variants (CNVs), 12 5′ and 3′ variants, 19 intronic variants, 5 nonsense variants, 1 frameshift deletion variant, 6 synonymous variants, 1 in-frame duplication, 3 gene conversions and 50 missense variants. Based upon a combination of clinical genetic and functional analysis, population data and in silico analysis, we classified 26 variants (all 3 CNVs, the in-frame duplication, all 3 gene conversions and 19 missense) as “pathogenic”, 3 variants (missense) as “likely pathogenic”, 5 variants (four missense and one promoter) as “predisposing”, 13 variants (all missense) as “unknown significance”, 2 variants (missense) as “likely benign”, and all remaining 51 variants as “benign”. Conclusions: We describe an expert classification of the 100 PRSS1 variants reported to date. The results have immediate implications for reclassifying many ClinVar-registered PRSS1 variants as well as providing optimal guidelines/standards for reporting PRSS1 variants.

KW - Chronic pancreatitis

KW - Genetic predisposition to disease

KW - PRSS1 gene

KW - Trypsinogen/trypsin

KW - Variant classification

UR - https://www.scopus.com/pages/publications/85159258595

U2 - 10.1016/j.pan.2023.04.004

DO - 10.1016/j.pan.2023.04.004

M3 - 文章

C2 - 37581535

AN - SCOPUS:85159258595

SN - 1424-3903

VL - 23

SP - 491

EP - 506

JO - Pancreatology

JF - Pancreatology

IS - 5

ER -

Classification of PRSS1 variants responsible for chronic pancreatitis: An expert perspective from the Franco-Chinese GREPAN Study Group

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联合国可持续发展目标

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