Obesity Variants in the GIPR Gene Are not Associated With Risk of Fracture or Bone Mineral Density

Author:

Styrkarsdottir Unnur1ORCID,Tragante Vinicius1ORCID,Stefansdottir Lilja1,Thorleifsson Gudmar1ORCID,Oddsson Asmundur1ORCID,Sørensen Erik2,Erikstrup Christian34ORCID,Schwarz Peter56,Jørgensen Henrik Løvendahl57,Lauritzen Jes Bruun8,Brunak Søren9ORCID,Knowlton Kirk U10,Nadauld Lincoln D11,Ullum Henrik12ORCID,Pedersen Ole Birger Vesterager513,Ostrowski Sisse Rye25,Holm Hilma1ORCID,Gudbjartsson Daniel F114,Sulem Patrick1ORCID,Stefansson Kari115ORCID

Affiliation:

1. Population Genomics, deCODE genetics/Amgen Inc , Reykjavik 102 , Iceland

2. Department of Clinical Immunology, Copenhagen University Hospital , Rigshospitalet, Copenhagen 2100 , Denmark

3. Department of Clinical Immunology, Aarhus University Hospital , Aarhus 8200 , Denmark

4. Department of Clinical Medicine, Aarhus University , Aarhus 8200 , Denmark

5. Department of Clinical Medicine, Faculty of Health and Medical Sciences, University of Copenhagen , Copenhagen 2200 , Denmark

6. Department of Endocrinology, Copenhagen University Hospital , Rigshospitalet, Copenhagen 2100 , Denmark

7. Department of Clinical Biochemistry, Amager Hvidovre Hospital , Copenhagen 2650 , Denmark

8. Department of Orthopedic Surgery, Bispebjerg Hospital, University of Copenhagen , Copenhagen 2400 , Denmark

9. Novo Nordisk Foundation Center for Protein Research, University of Copenhagen , Copenhagen 2200 , Denmark

10. Intermountain Health, Heart Institute , Salt Lake City, UT 84143 , USA

11. Intermountain Health, Cancer Center , St.George, UT 84790 , USA

12. Statens Serum Institut , Copenhagen 2300 , Denmark

13. Department of Clinical Immunology, Zealand University Hospital , Køge 4600 , Denmark

14. School of Engineering and Natural Sciences, University of Iceland , Reykjavik 102 , Iceland

15. Faculty of Medicine, School of Health Science, University of Iceland , Reykjavik 102 , Iceland

Abstract

Abstract Context It is not clear if antagonizing the GIP (glucose-dependent insulinotropic polypeptide) receptor (GIPR) for treatment of obesity is likely to increase the risk of fractures, or to lower bone mineral density (BMD) beyond what is expected with rapid weight loss. Objective The objective of this study was to investigate the risk of fracture and BMD of sequence variants in GIPR that reduce the activity of the GIP receptor and have been associated with reduced body mass index (BMI). Methods We analyzed the association of 3 missense variants in GIPR, a common variant, rs1800437 (p.Glu354Gln), and 2 rare variants, rs139215588 (p.Arg190Gln) and rs143430880 (p.Glu288Gly), as well as a burden of predicted loss-of-function (LoF) variants with risk of fracture and with BMD in a large meta-analysis of up to 1.2 million participants. We analyzed associations with fractures at different skeletal sites in the general population: any fractures, hip fractures, vertebral fractures and forearm fractures, and specifically nonvertebral and osteoporotic fractures in postmenopausal women. We also evaluated associations with BMD at the lumbar spine, femoral neck, and total body measured with dual-energy x-ray absorptiometry (DXA), and with BMD estimated from heel ultrasound (eBMD). Results None of the 3 missense variants in GIPR was significantly associated with increased risk of fractures or with lower BMD. Burden of LoF variants in GIPR was not associated with fractures or with BMD measured with clinically validated DXA, but was associated with eBMD. Conclusion Missense variants in GIPR, or burden of LoF variants in the gene, are not associated with risk of fractures or with lower BMD.

Funder

Novo Nordisk Foundation

Aarhus University Hospital

Publisher

The Endocrine Society

Subject

Biochemistry (medical),Clinical Biochemistry,Endocrinology,Biochemistry,Endocrinology, Diabetes and Metabolism

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