LRRK2 but not ATG16L1 is associated with Paneth cell defect in Japanese Crohn’s disease patients

Ta Chiang Liu; Takeo Naito; Zhenqiu Liu; Kelli L. Vandussen; Talin Haritunians; Dalin Li; Katsuya Endo; Yosuke Kawai; Masao Nagasaki; Yoshitaka Kinouchi; Dermot P.B. McGovern; Tooru Shimosegawa; Yoichi Kakuta; Thaddeus S. Stappenbeck

doi:10.1172/jci.insight.91917

LRRK2 but not ATG16L1 is associated with Paneth cell defect in Japanese Crohn’s disease patients

Ta Chiang Liu, Takeo Naito, Zhenqiu Liu, Kelli L. Vandussen, Talin Haritunians, Dalin Li, Katsuya Endo, Yosuke Kawai, Masao Nagasaki, Yoshitaka Kinouchi, Dermot P.B. McGovern, Tooru Shimosegawa, Yoichi Kakuta, Thaddeus S. Stappenbeck

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Abstract

BACKGROUND. Morphological patterns of Paneth cells are a prognostic biomarker in Western Crohn’s disease (CD) patients, and are associated with autophagy-associated ATG16L1 and NOD2 variants. We hypothesized that genetic determinants of Paneth cell phenotype in other ethnic CD cohorts are distinct but also involved in autophagy. METHODS. We performed a hypothesis-driven analysis of 56 single nucleotide polymorphisms (SNPs) associated with CD susceptibility or known to affect Paneth cell function in 110 Japanese CD patients who underwent ileal resection. We subsequently performed a genome-wide association analysis. Paneth cell phenotype was determined by defensin-5 immunofluorescence. Selected genotype–Paneth cell defect correlations were compared to a Western CD cohort (n = 164). RESULTS. The average percentage of abnormal Paneth cells in Japanese CD was similar to Western CD (P = 0.87), and abnormal Paneth cell phenotype was also associated with early recurrence (P = 0.013). In contrast to Western CD, ATG16L1 T300A was not associated with Paneth cell defect in Japanese CD (P = 0.20). Among the 56 selected SNPs, only LRRK2 M2397T showed significant association with Paneth cell defect (P = 3.62 × 10^–4), whereas in the Western CD cohort it was not (P = 0.76). Pathway analysis of LRRK2 and other candidate genes with P less than 5 × 10^–4 showed connections with known CD susceptibility genes and links to autophagy and TNF-α networks. CONCLUSIONS. We found dichotomous effects of ATG16L1 and LRRK2 on Paneth cell defect between Japanese and Western CD. Genes affecting Paneth cell phenotype in Japanese CD were also associated with autophagy. Paneth cell phenotype also predicted prognosis in Japanese CD.

Original language	English (US)
Article number	e91917
Journal	JCI Insight
Volume	2
Issue number	6
DOIs	https://doi.org/10.1172/jci.insight.91917
State	Published - Mar 23 2017

All Science Journal Classification (ASJC) codes

Medicine(all)

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10.1172/jci.insight.91917

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Liu, T. C., Naito, T., Liu, Z., Vandussen, K. L., Haritunians, T., Li, D., Endo, K., Kawai, Y., Nagasaki, M., Kinouchi, Y., McGovern, D. P. B., Shimosegawa, T., Kakuta, Y., & Stappenbeck, T. S. (2017). LRRK2 but not ATG16L1 is associated with Paneth cell defect in Japanese Crohn’s disease patients. JCI Insight, 2(6), Article e91917. https://doi.org/10.1172/jci.insight.91917

@article{78f044a2c986442e928249e633224a4c,

title = "LRRK2 but not ATG16L1 is associated with Paneth cell defect in Japanese Crohn{\textquoteright}s disease patients",

abstract = "BACKGROUND. Morphological patterns of Paneth cells are a prognostic biomarker in Western Crohn{\textquoteright}s disease (CD) patients, and are associated with autophagy-associated ATG16L1 and NOD2 variants. We hypothesized that genetic determinants of Paneth cell phenotype in other ethnic CD cohorts are distinct but also involved in autophagy. METHODS. We performed a hypothesis-driven analysis of 56 single nucleotide polymorphisms (SNPs) associated with CD susceptibility or known to affect Paneth cell function in 110 Japanese CD patients who underwent ileal resection. We subsequently performed a genome-wide association analysis. Paneth cell phenotype was determined by defensin-5 immunofluorescence. Selected genotype–Paneth cell defect correlations were compared to a Western CD cohort (n = 164). RESULTS. The average percentage of abnormal Paneth cells in Japanese CD was similar to Western CD (P = 0.87), and abnormal Paneth cell phenotype was also associated with early recurrence (P = 0.013). In contrast to Western CD, ATG16L1 T300A was not associated with Paneth cell defect in Japanese CD (P = 0.20). Among the 56 selected SNPs, only LRRK2 M2397T showed significant association with Paneth cell defect (P = 3.62 × 10–4), whereas in the Western CD cohort it was not (P = 0.76). Pathway analysis of LRRK2 and other candidate genes with P less than 5 × 10–4 showed connections with known CD susceptibility genes and links to autophagy and TNF-α networks. CONCLUSIONS. We found dichotomous effects of ATG16L1 and LRRK2 on Paneth cell defect between Japanese and Western CD. Genes affecting Paneth cell phenotype in Japanese CD were also associated with autophagy. Paneth cell phenotype also predicted prognosis in Japanese CD.",

author = "Liu, {Ta Chiang} and Takeo Naito and Zhenqiu Liu and Vandussen, {Kelli L.} and Talin Haritunians and Dalin Li and Katsuya Endo and Yosuke Kawai and Masao Nagasaki and Yoshitaka Kinouchi and McGovern, {Dermot P.B.} and Tooru Shimosegawa and Yoichi Kakuta and Stappenbeck, {Thaddeus S.}",

note = "Funding Information: received research grants from Toshiba Corporation during the conduct of the study. Funding Information: The study was supported by the Helmsley Charitable Trust (D.P.B.M., T.S.S.), Doris Duke Charitable Foundation grant 2014103 (T.C.L.), Crohn?s and Colitis Foundation grant 274415, NIH grants 1R56DK095820 (D.P.B.M., T.S.S.) and K01DK109081 (K.L.V.), NIH/National Center for Advancing Translational Sciences (NCATS) grant UL1 TR000448 (T.C.L.), and Japan Society for the Promotion of Science KAKENHI grants JP15H04805 and JP15K15284 (Y.K.). Computational resources for genotype imputation were provided by the Tohoku Medical Megabank Organization supercomputer system. Funding Information: FUNDING. Helmsley Charitable Trust, Doris Duke Foundation (grant 2014103), Japan Society for the Promotion of Science (KAKENHI grants JP15H04805 and JP15K15284), Crohn{\textquoteright}s and Colitis Foundation grant 274415, NIH (grants 1R56DK095820, K01DK109081, and UL1 TR000448). Funding Information: The study was supported by the Helmsley Charitable Trust (D.P.B.M., T.S.S.), Doris Duke Charitable Foundation grant 2014103 (T.C.L.), Crohn{\textquoteright}s and Colitis Foundation grant 274415, NIH grants 1R56DK095820 (D.P.B.M., T.S.S.) and K01DK109081 (K.L.V.), NIH/National Center for Advancing Translational Sciences (NCATS) grant UL1 TR000448 (T.C.L.), and Japan Society for the Promotion of Science KAKENHI grants JP15H04805 and JP15K15284 (Y.K.). Computational resources for genotype imputation were provided by the Tohoku Medical Megabank Organization supercomputer system. Publisher Copyright: {\textcopyright} 2017 American Society for Clinical Investigation. All rights reserved.",

year = "2017",

month = mar,

day = "23",

doi = "10.1172/jci.insight.91917",

language = "English (US)",

volume = "2",

journal = "JCI Insight",

issn = "2379-3708",

publisher = "The American Society for Clinical Investigation",

number = "6",

}

TY - JOUR

T1 - LRRK2 but not ATG16L1 is associated with Paneth cell defect in Japanese Crohn’s disease patients

AU - Liu, Ta Chiang

AU - Naito, Takeo

AU - Liu, Zhenqiu

AU - Vandussen, Kelli L.

AU - Haritunians, Talin

AU - Li, Dalin

AU - Endo, Katsuya

AU - Kawai, Yosuke

AU - Nagasaki, Masao

AU - Kinouchi, Yoshitaka

AU - McGovern, Dermot P.B.

AU - Shimosegawa, Tooru

AU - Kakuta, Yoichi

AU - Stappenbeck, Thaddeus S.

N1 - Funding Information: received research grants from Toshiba Corporation during the conduct of the study. Funding Information: The study was supported by the Helmsley Charitable Trust (D.P.B.M., T.S.S.), Doris Duke Charitable Foundation grant 2014103 (T.C.L.), Crohn?s and Colitis Foundation grant 274415, NIH grants 1R56DK095820 (D.P.B.M., T.S.S.) and K01DK109081 (K.L.V.), NIH/National Center for Advancing Translational Sciences (NCATS) grant UL1 TR000448 (T.C.L.), and Japan Society for the Promotion of Science KAKENHI grants JP15H04805 and JP15K15284 (Y.K.). Computational resources for genotype imputation were provided by the Tohoku Medical Megabank Organization supercomputer system. Funding Information: FUNDING. Helmsley Charitable Trust, Doris Duke Foundation (grant 2014103), Japan Society for the Promotion of Science (KAKENHI grants JP15H04805 and JP15K15284), Crohn’s and Colitis Foundation grant 274415, NIH (grants 1R56DK095820, K01DK109081, and UL1 TR000448). Funding Information: The study was supported by the Helmsley Charitable Trust (D.P.B.M., T.S.S.), Doris Duke Charitable Foundation grant 2014103 (T.C.L.), Crohn’s and Colitis Foundation grant 274415, NIH grants 1R56DK095820 (D.P.B.M., T.S.S.) and K01DK109081 (K.L.V.), NIH/National Center for Advancing Translational Sciences (NCATS) grant UL1 TR000448 (T.C.L.), and Japan Society for the Promotion of Science KAKENHI grants JP15H04805 and JP15K15284 (Y.K.). Computational resources for genotype imputation were provided by the Tohoku Medical Megabank Organization supercomputer system. Publisher Copyright: © 2017 American Society for Clinical Investigation. All rights reserved.

PY - 2017/3/23

Y1 - 2017/3/23

N2 - BACKGROUND. Morphological patterns of Paneth cells are a prognostic biomarker in Western Crohn’s disease (CD) patients, and are associated with autophagy-associated ATG16L1 and NOD2 variants. We hypothesized that genetic determinants of Paneth cell phenotype in other ethnic CD cohorts are distinct but also involved in autophagy. METHODS. We performed a hypothesis-driven analysis of 56 single nucleotide polymorphisms (SNPs) associated with CD susceptibility or known to affect Paneth cell function in 110 Japanese CD patients who underwent ileal resection. We subsequently performed a genome-wide association analysis. Paneth cell phenotype was determined by defensin-5 immunofluorescence. Selected genotype–Paneth cell defect correlations were compared to a Western CD cohort (n = 164). RESULTS. The average percentage of abnormal Paneth cells in Japanese CD was similar to Western CD (P = 0.87), and abnormal Paneth cell phenotype was also associated with early recurrence (P = 0.013). In contrast to Western CD, ATG16L1 T300A was not associated with Paneth cell defect in Japanese CD (P = 0.20). Among the 56 selected SNPs, only LRRK2 M2397T showed significant association with Paneth cell defect (P = 3.62 × 10–4), whereas in the Western CD cohort it was not (P = 0.76). Pathway analysis of LRRK2 and other candidate genes with P less than 5 × 10–4 showed connections with known CD susceptibility genes and links to autophagy and TNF-α networks. CONCLUSIONS. We found dichotomous effects of ATG16L1 and LRRK2 on Paneth cell defect between Japanese and Western CD. Genes affecting Paneth cell phenotype in Japanese CD were also associated with autophagy. Paneth cell phenotype also predicted prognosis in Japanese CD.

AB - BACKGROUND. Morphological patterns of Paneth cells are a prognostic biomarker in Western Crohn’s disease (CD) patients, and are associated with autophagy-associated ATG16L1 and NOD2 variants. We hypothesized that genetic determinants of Paneth cell phenotype in other ethnic CD cohorts are distinct but also involved in autophagy. METHODS. We performed a hypothesis-driven analysis of 56 single nucleotide polymorphisms (SNPs) associated with CD susceptibility or known to affect Paneth cell function in 110 Japanese CD patients who underwent ileal resection. We subsequently performed a genome-wide association analysis. Paneth cell phenotype was determined by defensin-5 immunofluorescence. Selected genotype–Paneth cell defect correlations were compared to a Western CD cohort (n = 164). RESULTS. The average percentage of abnormal Paneth cells in Japanese CD was similar to Western CD (P = 0.87), and abnormal Paneth cell phenotype was also associated with early recurrence (P = 0.013). In contrast to Western CD, ATG16L1 T300A was not associated with Paneth cell defect in Japanese CD (P = 0.20). Among the 56 selected SNPs, only LRRK2 M2397T showed significant association with Paneth cell defect (P = 3.62 × 10–4), whereas in the Western CD cohort it was not (P = 0.76). Pathway analysis of LRRK2 and other candidate genes with P less than 5 × 10–4 showed connections with known CD susceptibility genes and links to autophagy and TNF-α networks. CONCLUSIONS. We found dichotomous effects of ATG16L1 and LRRK2 on Paneth cell defect between Japanese and Western CD. Genes affecting Paneth cell phenotype in Japanese CD were also associated with autophagy. Paneth cell phenotype also predicted prognosis in Japanese CD.

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U2 - 10.1172/jci.insight.91917

DO - 10.1172/jci.insight.91917

M3 - Article

C2 - 28352666

AN - SCOPUS:85032615052

SN - 2379-3708

VL - 2

JO - JCI Insight

JF - JCI Insight

IS - 6

M1 - e91917

ER -

LRRK2 but not ATG16L1 is associated with Paneth cell defect in Japanese Crohn’s disease patients

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