The genetics of non-monogenic IBD

被引:19
作者
Jans, Deborah [1 ]
Cleynen, Isabelle [1 ]
机构
[1] Katholieke Univ Leuven, Dept Human Genet, Lab Complex Genet, Herestr 49, box610, B-3000 Louvain, Belgium
来源
HUMAN GENETICS | 2023年 / 142卷 / 05期
关键词
INFLAMMATORY-BOWEL-DISEASE; GENOME-WIDE ASSOCIATION; ULCERATIVE-COLITIS PATIENTS; CROHNS-DISEASE; SUSCEPTIBILITY LOCI; HLA DRB1-ASTERISK-0103; AFRICAN-AMERICANS; RISK PREDICTION; COMPLEX DISEASE; CLINICAL-COURSE;
D O I
10.1007/s00439-023-02521-9
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Inflammatory bowel disease (IBD), with Crohn's disease and ulcerative colitis as main subtypes, is a prototypical multifactorial disease with both genetic and environmental factors involved. Genetically, IBD covers a wide spectrum from monogenic to polygenic forms. In polygenic disease, many genetic variants each contribute a small amount to disease risk. With the advent of genome-wide association studies (GWAS), it became possible to find these variants and corresponding genes, leading so far to the discovery of ca 240 loci associated with IBD. Together, these however explain only 20-25% of the heritability of IBD, leaving a large portion unaccounted for. This missing heritability might be hidden in common variants with even lower effect than the ones currently found through GWAS, but also in rare variants which can be found through large-scale sequencing studies or potentially in multiplex families. In this review, we will give an overview of the current knowledge about the genetics of non-monogenic IBD and how it differs from the monogenic form(s), and future perspectives. The history of IBD genetic studies from twin studies over linkage studies to GWAS, and finally large-scale sequencing studies and the revisiting of multiplex families will be discussed.
引用
收藏
页码:669 / 682
页数:14
相关论文
共 84 条
  • [1] Mutations in NOD2 are associated with fibrostenosing disease in patients with Crohn's disease
    Abreu, MT
    Taylor, KD
    Lin, YC
    Hang, T
    Gaiennie, J
    Landers, CJ
    Vasiliauskas, EA
    Kam, LY
    Rojany, M
    Papadakis, KA
    Rotter, JI
    Targan, SR
    Yang, HY
    [J]. GASTROENTEROLOGY, 2002, 123 (03) : 679 - 688
  • [2] Evaluating empirical bounds on complex disease genetic architecture
    Agarwala, Vineeta
    Flannick, Jason
    Sunyaev, Shamil
    Altshuler, David
    [J]. NATURE GENETICS, 2013, 45 (12) : 1418 - U167
  • [3] Meta-analysis identifies 29 additional ulcerative colitis risk loci, increasing the number of confirmed associations to 47
    Anderson, Carl A.
    Boucher, Gabrielle
    Lees, Charlie W.
    Franke, Andre
    D'Amato, Mauro
    Taylor, Kent D.
    Lee, James C.
    Goyette, Philippe
    Imielinski, Marcin
    Latiano, Anna
    Lagace, Caroline
    Scott, Regan
    Amininejad, Leila
    Bumpstead, Suzannah
    Baidoo, Leonard
    Baldassano, Robert N.
    Barclay, Murray
    Bayless, Theodore M.
    Brand, Stephan
    Buening, Carsten
    Colombel, Jean-Frederic
    Denson, Lee A.
    De Vos, Martine
    Dubinsky, Marla
    Edwards, Cathryn
    Ellinghaus, David
    Fehrmann, Rudolf S. N.
    Floyd, James A. B.
    Florin, Timothy
    Franchimont, Denis
    Franke, Lude
    Georges, Michel
    Glas, Juergen
    Glazer, Nicole L.
    Guthery, Stephen L.
    Haritunians, Talin
    Hayward, Nicholas K.
    Hugot, Jean-Pierre
    Jobin, Gilles
    Laukens, Debby
    Lawrance, Ian
    Lemann, Marc
    Levine, Arie
    Libioulle, Cecile
    Louis, Edouard
    McGovern, Dermot P.
    Milla, Monica
    Montgomery, Grant W.
    Morley, Katherine I.
    Mowat, Craig
    [J]. NATURE GENETICS, 2011, 43 (03) : 246 - U94
  • [4] HLA-DRB1 alleles may influence disease phenotype in patients with inflammatory bowel disease: A critical reappraisal with review of the literature
    Annese, V
    Piepoli, A
    Latiano, A
    Lombardi, G
    Napolitano, G
    Caruso, N
    Cocchiara, E
    Accadia, L
    Perri, F
    Andriulli, A
    [J]. DISEASES OF THE COLON & RECTUM, 2005, 48 (01) : 57 - 64
  • [5] Understanding polygenic models, their development and the potential application of polygenic scores in healthcare
    Babb de Villiers, Chantal
    Kroese, Mark
    Moorthie, Sowmiya
    [J]. JOURNAL OF MEDICAL GENETICS, 2020, 57 (11) : 725 - 732
  • [6] Genome-wide association defines more than 30 distinct susceptibility loci for Crohn's disease
    Barrett, Jeffrey C.
    Hansoul, Sarah
    Nicolae, Dan L.
    Cho, Judy H.
    Duerr, Richard H.
    Rioux, John D.
    Brant, Steven R.
    Silverberg, Mark S.
    Taylor, Kent D.
    Barmada, M. Michael
    Bitton, Alain
    Dassopoulos, Themistocles
    Datta, Lisa Wu
    Green, Todd
    Griffiths, Anne M.
    Kistner, Emily O.
    Murtha, Michael T.
    Regueiro, Miguel D.
    Rotter, Jerome I.
    Schumm, L. Philip
    Steinhart, A. Hillary
    Targan, Stephan R.
    Xavier, Ramnik J.
    Libioulle, Cecile
    Sandor, Cynthia
    Lathrop, Mark
    Belaiche, Jacques
    Dewit, Olivier
    Gut, Ivo
    Heath, Simon
    Laukens, Debby
    Mni, Myriam
    Rutgeerts, Paul
    Van Gossum, Andre
    Zelenika, Diana
    Franchimont, Denis
    Hugot, Jean-Pierre
    de Vos, Martine
    Vermeire, Severine
    Louis, Edouard
    Cardon, Lon R.
    Anderson, Carl A.
    Drummond, Hazel
    Nimmo, Elaine
    Ahmad, Tariq
    Prescott, Natalie J.
    Onnie, Clive M.
    Fisher, Sheila A.
    Marchini, Jonathan
    Ghori, Jilur
    [J]. NATURE GENETICS, 2008, 40 (08) : 955 - 962
  • [7] Genome-wide association study of ulcerative colitis identifies three new susceptibility loci, including the HNF4A region
    Barrett, Jeffrey C.
    Lee, James C.
    Lees, Charles W.
    Prescott, Natalie J.
    Anderson, Carl A.
    Phillips, Anne
    Wesley, Emma
    Parnell, Kirstie
    Zhang, Hu
    Drummond, Hazel
    Nimmo, Elaine R.
    Massey, Dunecan
    Blaszczyk, Kasia
    Elliott, Timothy
    Cotterill, Lynn
    Dallal, Helen
    Lobo, Alan J.
    Mowat, Craig
    Sanderson, Jeremy D.
    Jewell, Derek P.
    Newman, William G.
    Edwards, Cathryn
    Ahmad, Tariq
    Mansfield, John C.
    Satsangi, Jack
    Parkes, Miles
    Mathew, Christopher G.
    Donnelly, Peter
    Peltonen, Leena
    Blackwell, Jenefer M.
    Bramon, Elvira
    Brown, Matthew A.
    Casas, Juan P.
    Corvin, Aiden
    Craddock, Nicholas
    Deloukas, Panos
    Duncanson, Audrey
    Jankowski, Janusz
    Markus, Hugh S.
    McCarthy, Mark I.
    Palmer, Colin N. A.
    Plomin, Robert
    Rautanen, Anna
    Sawcer, Stephen J.
    Samani, Nilesh
    Trembath, Richard C.
    Viswanathan, Ananth C.
    Wood, Nicholas
    Spencer, Chris C. A.
    Bellenguez, Celine
    [J]. NATURE GENETICS, 2009, 41 (12) : 1330 - U99
  • [8] Differences in Clinical Course, Genetics, and the Microbiome Between Familial and Sporadic Inflammatory Bowel Diseases
    Borren, Nienke Z.
    Conway, Grace
    Garber, John J.
    Khalili, Hamed
    Budree, Shrish
    Mallick, Himel
    Yajnik, Vijay
    Xavier, Ramnik J.
    Ananthakrishnan, Ashwin N.
    [J]. JOURNAL OF CROHNS & COLITIS, 2018, 12 (05) : 525 - 531
  • [9] Evidence for genetic heterogeneity in inflammatory bowel disease (IBD); HLA genes in the predisposition to suffer from ulcerative colitis (UC) and Crohn's disease (CD)
    Bouma, G
    Pool, MO
    Crusius, JBA
    Schreuder, GMT
    Hellemans, HPR
    Meijer, BUGA
    Kostense, PJ
    Giphart, MJ
    Meuwissen, SGM
    Pena, AS
    [J]. CLINICAL AND EXPERIMENTAL IMMUNOLOGY, 1997, 109 (01) : 175 - 179
  • [10] Defining complex contributions of NOD2/CARD15 gene mutations, age at onset, and tobacco use on Crohn's disease phenotypes
    Brant, SR
    Picco, MF
    Achkar, JP
    Bayless, TM
    Kane, SV
    Brzezinski, A
    Nouvet, FJ
    Bonen, D
    Karban, A
    Dassopoulos, T
    Karaliukas, R
    Beaty, TH
    Hanauer, SB
    Duerr, RH
    Cho, JH
    [J]. INFLAMMATORY BOWEL DISEASES, 2003, 9 (05) : 281 - 289
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