Identification of four novel genes contributing to familial elevated plasma HDL cholesterol in humans

Roshni R. Singaraja; Ian Tietjen; G. Kees Hovingh; Patrick L. Franchini; Chris Radomski; Kenny Wong; Margaret vanHeek; Ioannis M. Stylianou; Linus Lin; Liangsu Wang; Lyndon Mitnaul; Brian Hubbard; Michael Winther; Maryanne Mattice; Annick Legendre; Robin Sherrington; John J. Kastelein; Karen Akinsanya; Andrew Plump; Michael R. Hayden

doi:https://doi.org/10.1194/jlr.M048710

Identification of four novel genes contributing to familial elevated plasma HDL cholesterol in humans

Roshni R. Singaraja, Ian Tietjen, G. Kees Hovingh, Patrick L. Franchini, Chris Radomski, Kenny Wong, Margaret vanHeek, Ioannis M. Stylianou, Linus Lin, Liangsu Wang, Lyndon Mitnaul, Brian Hubbard, Michael Winther, Maryanne Mattice, Annick Legendre, Robin Sherrington, John J. Kastelein, Karen Akinsanya, Andrew Plump, Michael R. Hayden

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

23 Citations (Scopus)

Abstract

While genetic determinants strongly influence HDL cholesterol (HDLc) levels, most genetic causes underlying variation in HDLc remain unknown. We aimed to identify novel rare mutations with large effects in candidate genes contributing to extreme HDLc in humans, utilizing family-based Mendelian genetics. We performed next-generation sequencing of 456 candidate HDLc-regulating genes in 200 unrelated probands with extremely low ( <= 10th percentile) or high (>= 90th percentile) HDLc. Probands were excluded if known mutations existed in the established HDLc-regulating genes ABCA1, APOA1, LCAT, cholesteryl ester transfer protein (CETP), endothelial lipase (LIPG), and UDP-N-acetyl-alpha-D-galactosamine: polypeptide N-acetylgalactosaminyltransferase 2 (GALNT2). We identified 93 novel coding or splice-site variants in 72 candidate genes. Each variant was genotyped in the proband's family. Family-based association analyses were performed for variants with sufficient power to detect significance at P <0.05 with a total of 627 family members being assessed. Mutations in the genes glucokinase regulatory protein (GCKR), RNase L (RNASEL), leukocyte immunoglobulin-like receptor 3 (LILRA3), and dynein axonemal heavy chain 10 (DNAH10) segregated with elevated HDLc levels in families, while no mutations associated with low HDLc. Taken together, we have identified mutations in four novel genes that may play a role in regulating HDLc levels in humans

Original language	English
Pages (from-to)	1693-1701
Journal	Journal of Lipid Research
Volume	55
Issue number	8
DOIs	https://doi.org/10.1194/jlr.M048710
Publication status	Published - 2014

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https://doi.org/10.1194/jlr.M048710

Cite this

Singaraja, R. R., Tietjen, I., Hovingh, G. K., Franchini, P. L., Radomski, C., Wong, K., vanHeek, M., Stylianou, I. M., Lin, L., Wang, L., Mitnaul, L., Hubbard, B., Winther, M., Mattice, M., Legendre, A., Sherrington, R., Kastelein, J. J., Akinsanya, K., Plump, A., & Hayden, M. R. (2014). Identification of four novel genes contributing to familial elevated plasma HDL cholesterol in humans. Journal of Lipid Research, 55(8), 1693-1701. https://doi.org/10.1194/jlr.M048710

@article{604b19ea5ce143bf8266b19d1eb97823,

title = "Identification of four novel genes contributing to familial elevated plasma HDL cholesterol in humans",

abstract = "While genetic determinants strongly influence HDL cholesterol (HDLc) levels, most genetic causes underlying variation in HDLc remain unknown. We aimed to identify novel rare mutations with large effects in candidate genes contributing to extreme HDLc in humans, utilizing family-based Mendelian genetics. We performed next-generation sequencing of 456 candidate HDLc-regulating genes in 200 unrelated probands with extremely low ( <= 10th percentile) or high (>= 90th percentile) HDLc. Probands were excluded if known mutations existed in the established HDLc-regulating genes ABCA1, APOA1, LCAT, cholesteryl ester transfer protein (CETP), endothelial lipase (LIPG), and UDP-N-acetyl-alpha-D-galactosamine: polypeptide N-acetylgalactosaminyltransferase 2 (GALNT2). We identified 93 novel coding or splice-site variants in 72 candidate genes. Each variant was genotyped in the proband's family. Family-based association analyses were performed for variants with sufficient power to detect significance at P <0.05 with a total of 627 family members being assessed. Mutations in the genes glucokinase regulatory protein (GCKR), RNase L (RNASEL), leukocyte immunoglobulin-like receptor 3 (LILRA3), and dynein axonemal heavy chain 10 (DNAH10) segregated with elevated HDLc levels in families, while no mutations associated with low HDLc. Taken together, we have identified mutations in four novel genes that may play a role in regulating HDLc levels in humans",

author = "Singaraja, {Roshni R.} and Ian Tietjen and Hovingh, {G. Kees} and Franchini, {Patrick L.} and Chris Radomski and Kenny Wong and Margaret vanHeek and Stylianou, {Ioannis M.} and Linus Lin and Liangsu Wang and Lyndon Mitnaul and Brian Hubbard and Michael Winther and Maryanne Mattice and Annick Legendre and Robin Sherrington and Kastelein, {John J.} and Karen Akinsanya and Andrew Plump and Hayden, {Michael R.}",

year = "2014",

doi = "https://doi.org/10.1194/jlr.M048710",

language = "English",

volume = "55",

pages = "1693--1701",

journal = "Journal of Lipid Research",

issn = "0022-2275",

publisher = "American Society for Biochemistry and Molecular Biology Inc.",

number = "8",

}

Singaraja, RR, Tietjen, I, Hovingh, GK, Franchini, PL, Radomski, C, Wong, K, vanHeek, M, Stylianou, IM, Lin, L, Wang, L, Mitnaul, L, Hubbard, B, Winther, M, Mattice, M, Legendre, A, Sherrington, R, Kastelein, JJ, Akinsanya, K, Plump, A & Hayden, MR 2014, 'Identification of four novel genes contributing to familial elevated plasma HDL cholesterol in humans', Journal of Lipid Research, vol. 55, no. 8, pp. 1693-1701. https://doi.org/10.1194/jlr.M048710

TY - JOUR

T1 - Identification of four novel genes contributing to familial elevated plasma HDL cholesterol in humans

AU - Singaraja, Roshni R.

AU - Tietjen, Ian

AU - Hovingh, G. Kees

AU - Franchini, Patrick L.

AU - Radomski, Chris

AU - Wong, Kenny

AU - vanHeek, Margaret

AU - Stylianou, Ioannis M.

AU - Lin, Linus

AU - Wang, Liangsu

AU - Mitnaul, Lyndon

AU - Hubbard, Brian

AU - Winther, Michael

AU - Mattice, Maryanne

AU - Legendre, Annick

AU - Sherrington, Robin

AU - Kastelein, John J.

AU - Akinsanya, Karen

AU - Plump, Andrew

AU - Hayden, Michael R.

PY - 2014

Y1 - 2014

N2 - While genetic determinants strongly influence HDL cholesterol (HDLc) levels, most genetic causes underlying variation in HDLc remain unknown. We aimed to identify novel rare mutations with large effects in candidate genes contributing to extreme HDLc in humans, utilizing family-based Mendelian genetics. We performed next-generation sequencing of 456 candidate HDLc-regulating genes in 200 unrelated probands with extremely low ( <= 10th percentile) or high (>= 90th percentile) HDLc. Probands were excluded if known mutations existed in the established HDLc-regulating genes ABCA1, APOA1, LCAT, cholesteryl ester transfer protein (CETP), endothelial lipase (LIPG), and UDP-N-acetyl-alpha-D-galactosamine: polypeptide N-acetylgalactosaminyltransferase 2 (GALNT2). We identified 93 novel coding or splice-site variants in 72 candidate genes. Each variant was genotyped in the proband's family. Family-based association analyses were performed for variants with sufficient power to detect significance at P <0.05 with a total of 627 family members being assessed. Mutations in the genes glucokinase regulatory protein (GCKR), RNase L (RNASEL), leukocyte immunoglobulin-like receptor 3 (LILRA3), and dynein axonemal heavy chain 10 (DNAH10) segregated with elevated HDLc levels in families, while no mutations associated with low HDLc. Taken together, we have identified mutations in four novel genes that may play a role in regulating HDLc levels in humans

AB - While genetic determinants strongly influence HDL cholesterol (HDLc) levels, most genetic causes underlying variation in HDLc remain unknown. We aimed to identify novel rare mutations with large effects in candidate genes contributing to extreme HDLc in humans, utilizing family-based Mendelian genetics. We performed next-generation sequencing of 456 candidate HDLc-regulating genes in 200 unrelated probands with extremely low ( <= 10th percentile) or high (>= 90th percentile) HDLc. Probands were excluded if known mutations existed in the established HDLc-regulating genes ABCA1, APOA1, LCAT, cholesteryl ester transfer protein (CETP), endothelial lipase (LIPG), and UDP-N-acetyl-alpha-D-galactosamine: polypeptide N-acetylgalactosaminyltransferase 2 (GALNT2). We identified 93 novel coding or splice-site variants in 72 candidate genes. Each variant was genotyped in the proband's family. Family-based association analyses were performed for variants with sufficient power to detect significance at P <0.05 with a total of 627 family members being assessed. Mutations in the genes glucokinase regulatory protein (GCKR), RNase L (RNASEL), leukocyte immunoglobulin-like receptor 3 (LILRA3), and dynein axonemal heavy chain 10 (DNAH10) segregated with elevated HDLc levels in families, while no mutations associated with low HDLc. Taken together, we have identified mutations in four novel genes that may play a role in regulating HDLc levels in humans

U2 - https://doi.org/10.1194/jlr.M048710

DO - https://doi.org/10.1194/jlr.M048710

M3 - Article

C2 - 24891332

SN - 0022-2275

VL - 55

SP - 1693

EP - 1701

JO - Journal of Lipid Research

JF - Journal of Lipid Research

IS - 8

ER -