Jacqueline S Dron1,2, Allison A Dilliott1,2, Arden Lawson1,2, Adam D McIntyre1, Brent D Davis3, Jian Wang1, Henian Cao1, Irina Movsesyan4, Mary J Malloy4, Clive R Pullinger4, John P Kane4, Robert A Hegele1,2,5. 1. From the Robarts Research Institute, Western University, London, ON, Canada (J.S.D., A.A.D., A.L., A.D.M., J.W., H.C., R.A.H.). 2. Department of Biochemistry, Western University, London, ON, Canada (J.S.D., A.A.D., A.L., R.A.H.). 3. Schulich School of Medicine and Dentistry, and Department of Computer Science, Western University, London, ON, Canada (B.D.D.). 4. Cardiovascular Research Institute, University of California San Francisco (I.M., M.J.M., C.R.P., J.P.K.). 5. Department of Medicine, Western University, London, ON, Canada (R.A.H.).
Abstract
OBJECTIVE: Genetic determinants of severe hypertriglyceridemia include both common variants with small effects (assessed using polygenic risk scores) plus heterozygous and homozygous rare variants in canonical genes directly affecting triglyceride metabolism. Here, we broadened our scope to detect associations with rare loss-of-function variants in genes affecting noncanonical pathways, including those known to affect triglyceride metabolism indirectly. Approach and Results: From targeted next-generation sequencing of 69 metabolism-related genes in 265 patients of European descent with severe hypertriglyceridemia (≥10 mmol/L or ≥885 mg/dL) and 477 normolipidemic controls, we focused on the association of rare heterozygous loss-of-function variants in individual genes. We observed that compared with controls, severe hypertriglyceridemia patients were 20.2× (95% CI, 1.11-366.1; P=0.03) more likely than controls to carry a rare loss-of-function variant in CREB3L3, which encodes a transcription factor that regulates several target genes with roles in triglyceride metabolism. CONCLUSIONS: Our findings indicate that rare variants in a noncanonical gene for triglyceride metabolism, namely CREB3L3, contribute significantly to severe hypertriglyceridemia. Secondary genes and pathways should be considered when evaluating the genetic architecture of this complex trait.
OBJECTIVE: Genetic determinants of severe hypertriglyceridemia include both common variants with small effects (assessed using polygenic risk scores) plus heterozygous and homozygous rare variants in canonical genes directly affecting triglyceride metabolism. Here, we broadened our scope to detect associations with rare loss-of-function variants in genes affecting noncanonical pathways, including those known to affect triglyceride metabolism indirectly. Approach and Results: From targeted next-generation sequencing of 69 metabolism-related genes in 265 patients of European descent with severe hypertriglyceridemia (≥10 mmol/L or ≥885 mg/dL) and 477 normolipidemic controls, we focused on the association of rare heterozygous loss-of-function variants in individual genes. We observed that compared with controls, severe hypertriglyceridemiapatients were 20.2× (95% CI, 1.11-366.1; P=0.03) more likely than controls to carry a rare loss-of-function variant in CREB3L3, which encodes a transcription factor that regulates several target genes with roles in triglyceride metabolism. CONCLUSIONS: Our findings indicate that rare variants in a noncanonical gene for triglyceride metabolism, namely CREB3L3, contribute significantly to severe hypertriglyceridemia. Secondary genes and pathways should be considered when evaluating the genetic architecture of this complex trait.
Authors: Masami Shimizu-Albergine; Debapriya Basu; Jenny E Kanter; Farah Kramer; Vishal Kothari; Shelley Barnhart; Carissa Thornock; Adam E Mullick; Noemie Clouet-Foraison; Tomas Vaisar; Jay W Heinecke; Robert A Hegele; Ira J Goldberg; Karin E Bornfeldt Journal: J Clin Invest Date: 2021-11-15 Impact factor: 14.808
Authors: George Hindy; Peter Dornbos; Mark D Chaffin; Dajiang J Liu; Minxian Wang; Margaret Sunitha Selvaraj; David Zhang; Joseph Park; Carlos A Aguilar-Salinas; Lucinda Antonacci-Fulton; Diego Ardissino; Donna K Arnett; Stella Aslibekyan; Gil Atzmon; Christie M Ballantyne; Francisco Barajas-Olmos; Nir Barzilai; Lewis C Becker; Lawrence F Bielak; Joshua C Bis; John Blangero; Eric Boerwinkle; Lori L Bonnycastle; Erwin Bottinger; Donald W Bowden; Matthew J Bown; Jennifer A Brody; Jai G Broome; Noël P Burtt; Brian E Cade; Federico Centeno-Cruz; Edmund Chan; Yi-Cheng Chang; Yii-Der I Chen; Ching-Yu Cheng; Won Jung Choi; Rajiv Chowdhury; Cecilia Contreras-Cubas; Emilio J Córdova; Adolfo Correa; L Adrienne Cupples; Joanne E Curran; John Danesh; Paul S de Vries; Ralph A DeFronzo; Harsha Doddapaneni; Ravindranath Duggirala; Susan K Dutcher; Patrick T Ellinor; Leslie S Emery; Jose C Florez; Myriam Fornage; Barry I Freedman; Valentin Fuster; Ma Eugenia Garay-Sevilla; Humberto García-Ortiz; Soren Germer; Richard A Gibbs; Christian Gieger; Benjamin Glaser; Clicerio Gonzalez; Maria Elena Gonzalez-Villalpando; Mariaelisa Graff; Sarah E Graham; Niels Grarup; Leif C Groop; Xiuqing Guo; Namrata Gupta; Sohee Han; Craig L Hanis; Torben Hansen; Jiang He; Nancy L Heard-Costa; Yi-Jen Hung; Mi Yeong Hwang; Marguerite R Irvin; Sergio Islas-Andrade; Gail P Jarvik; Hyun Min Kang; Sharon L R Kardia; Tanika Kelly; Eimear E Kenny; Alyna T Khan; Bong-Jo Kim; Ryan W Kim; Young Jin Kim; Heikki A Koistinen; Charles Kooperberg; Johanna Kuusisto; Soo Heon Kwak; Markku Laakso; Leslie A Lange; Jiwon Lee; Juyoung Lee; Seonwook Lee; Donna M Lehman; Rozenn N Lemaitre; Allan Linneberg; Jianjun Liu; Ruth J F Loos; Steven A Lubitz; Valeriya Lyssenko; Ronald C W Ma; Lisa Warsinger Martin; Angélica Martínez-Hernández; Rasika A Mathias; Stephen T McGarvey; Ruth McPherson; James B Meigs; Thomas Meitinger; Olle Melander; Elvia Mendoza-Caamal; Ginger A Metcalf; Xuenan Mi; Karen L Mohlke; May E Montasser; Jee-Young Moon; Hortensia Moreno-Macías; Alanna C Morrison; Donna M Muzny; Sarah C Nelson; Peter M Nilsson; Jeffrey R O'Connell; Marju Orho-Melander; Lorena Orozco; Colin N A Palmer; Nicholette D Palmer; Cheol Joo Park; Kyong Soo Park; Oluf Pedersen; Juan M Peralta; Patricia A Peyser; Wendy S Post; Michael Preuss; Bruce M Psaty; Qibin Qi; D C Rao; Susan Redline; Alexander P Reiner; Cristina Revilla-Monsalve; Stephen S Rich; Nilesh Samani; Heribert Schunkert; Claudia Schurmann; Daekwan Seo; Jeong-Sun Seo; Xueling Sim; Rob Sladek; Kerrin S Small; Wing Yee So; Adrienne M Stilp; E Shyong Tai; Claudia H T Tam; Kent D Taylor; Yik Ying Teo; Farook Thameem; Brian Tomlinson; Michael Y Tsai; Tiinamaija Tuomi; Jaakko Tuomilehto; Teresa Tusié-Luna; Miriam S Udler; Rob M van Dam; Ramachandran S Vasan; Karine A Viaud Martinez; Fei Fei Wang; Xuzhi Wang; Hugh Watkins; Daniel E Weeks; James G Wilson; Daniel R Witte; Tien-Yin Wong; Lisa R Yanek; Sekar Kathiresan; Daniel J Rader; Jerome I Rotter; Michael Boehnke; Mark I McCarthy; Cristen J Willer; Pradeep Natarajan; Jason A Flannick; Amit V Khera; Gina M Peloso Journal: Am J Hum Genet Date: 2021-12-20 Impact factor: 11.043