Cystatin C and risk of diabetes and the metabolic syndrome - Biomarker and genotype association analyses

Magnusson, Martin; Molvin, John; Engström, Gunnar; Svensson, Patrik; Persson, Margaretha; Christensson, Anders; Nilsson, Peter; Melander, Olle

Cystatin C and risk of diabetes and the metabolic syndrome - Biomarker and genotype association analyses

Mark

Magnusson, Martin ^LU

; Molvin, John ^LU ; Engström, Gunnar ^LU ; Svensson, Patrik ^LU ; Persson, Margaretha ^LU

; Christensson, Anders ^LU ; Nilsson, Peter ^LU and Melander, Olle ^LU

(2016) In PLoS ONE 11(5).

Abstract: Background We recently reported a relationship between plasma levels of cystatin C and incidence of the metabolic syndrome (MetS) among the first 2,369 subjects who participated in the reexamination study of the population-based Malmö and Diet Cancer Cardiovascular cohort (MDC-CC-re-exam). In this study we aimed to replicate these results and also investigate if cystatin C was causally associated with MetS and diabetes. Methods We estimated the effect size of the strongest GWAS derived cystatin C SNP (major allele of rs13038305) on plasma cystatin C in the now completed MDC-CC-re-exam (n = 3,734) and thereafter examined the association between plasma cystatin C (403 cases of diabetes and2665 controls) as well as rs13038305 (235 cases... (More); Background We recently reported a relationship between plasma levels of cystatin C and incidence of the metabolic syndrome (MetS) among the first 2,369 subjects who participated in the reexamination study of the population-based Malmö and Diet Cancer Cardiovascular cohort (MDC-CC-re-exam). In this study we aimed to replicate these results and also investigate if cystatin C was causally associated with MetS and diabetes. Methods We estimated the effect size of the strongest GWAS derived cystatin C SNP (major allele of rs13038305) on plasma cystatin C in the now completed MDC-CC-re-exam (n = 3,734) and thereafter examined the association between plasma cystatin C (403 cases of diabetes and2665 controls) as well as rs13038305 (235 cases and 2425 controls) with incident diabetes. The association of rs13038305 and incident MetS (511 cases of MetS and 1980 controls) was similarly investigated in the whole MDC-CC-re-exam. We also attempted to replicate our previously shown association of cystatin C with incident MetS in subjects from the MDC-CC-re-exam (147 cases and 711 controls) that were not included in our previous report. Results In the entire MDC-CC-re-exam, each copy of the major allele of rs13038305 was associated with approximately 0.30 standard deviation (SD) higher plasma concentration of cystatin C (β = 0.33, p = 4.2E-28 ) in age and sex adjusted analysis. Cystatin C in plasma was not associated with incident diabetes after adjustment for known diabetes risk factors (OR per 1 SD increment 0.99 (0.86-1.13), p = 0.842). In the replication cohort of MDC-CC-re-exam, the OR (95% CI) for incident MetS in subjects belonging to quartiles 1, 2, 3 and 4 of plasma cystatin C levels was 1.00 (reference), 1.21 (0.70-2.07), 1.62 (0.95-2.78) and 1.72 (1.01-2.93) (ptrend = 0.026) in age and sex adjusted analysis. In the entire MDC-CC-re-exam the odds ratio for incident MetS and diabetes per copy of the major rs13038305 allele was 1.13, (0.95-1.34), p = 0.160 and 1.07, 95% CI 0.89-1.30, p = 0.478, respectively. Conclusion We were able to replicate our previously shown association between high levels of cystatin C and increased risk of future development of MetS. However, a causal involvement of cystatin C in the etiology of MetS or diabetes seems unlikely since genetic elevation of plasma cystatin C was not significantly related to incidence of these diseases.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/5a86a4d5-5289-4cdb-8963-bed2b97aee32

author

Magnusson, Martin ^LU

; Molvin, John ^LU ; Engström, Gunnar ^LU ; Svensson, Patrik ^LU ; Persson, Margaretha ^LU

; Christensson, Anders ^LU ; Nilsson, Peter ^LU and Melander, Olle ^LU

organization

publishing date

2016-05-01

type

Contribution to journal

publication status

published

subject

Endocrinology and Diabetes

in

PLoS ONE

volume

11

issue

5

article number

e0155735

publisher

Public Library of Science (PLoS)

external identifiers

scopus:84971441133
pmid:27218257
wos:000376880700013

ISSN

1932-6203

DOI

10.1371/journal.pone.0155735

project

The use of Genomics and Proteomics for the Detection and Prevention of Cardiometabolic Disease

language

English

LU publication?

yes

id

5a86a4d5-5289-4cdb-8963-bed2b97aee32

date added to LUP

2016-06-29 09:15:26

date last changed

2024-07-12 12:50:58

@article{5a86a4d5-5289-4cdb-8963-bed2b97aee32,
  abstract     = {{<p>Background We recently reported a relationship between plasma levels of cystatin C and incidence of the metabolic syndrome (MetS) among the first 2,369 subjects who participated in the reexamination study of the population-based Malmö and Diet Cancer Cardiovascular cohort (MDC-CC-re-exam). In this study we aimed to replicate these results and also investigate if cystatin C was causally associated with MetS and diabetes. Methods We estimated the effect size of the strongest GWAS derived cystatin C SNP (major allele of rs13038305) on plasma cystatin C in the now completed MDC-CC-re-exam (n = 3,734) and thereafter examined the association between plasma cystatin C (403 cases of diabetes and2665 controls) as well as rs13038305 (235 cases and 2425 controls) with incident diabetes. The association of rs13038305 and incident MetS (511 cases of MetS and 1980 controls) was similarly investigated in the whole MDC-CC-re-exam. We also attempted to replicate our previously shown association of cystatin C with incident MetS in subjects from the MDC-CC-re-exam (147 cases and 711 controls) that were not included in our previous report. Results In the entire MDC-CC-re-exam, each copy of the major allele of rs13038305 was associated with approximately 0.30 standard deviation (SD) higher plasma concentration of cystatin C (β = 0.33, p = 4.2E-28 ) in age and sex adjusted analysis. Cystatin C in plasma was not associated with incident diabetes after adjustment for known diabetes risk factors (OR per 1 SD increment 0.99 (0.86-1.13), p = 0.842). In the replication cohort of MDC-CC-re-exam, the OR (95% CI) for incident MetS in subjects belonging to quartiles 1, 2, 3 and 4 of plasma cystatin C levels was 1.00 (reference), 1.21 (0.70-2.07), 1.62 (0.95-2.78) and 1.72 (1.01-2.93) (ptrend = 0.026) in age and sex adjusted analysis. In the entire MDC-CC-re-exam the odds ratio for incident MetS and diabetes per copy of the major rs13038305 allele was 1.13, (0.95-1.34), p = 0.160 and 1.07, 95% CI 0.89-1.30, p = 0.478, respectively. Conclusion We were able to replicate our previously shown association between high levels of cystatin C and increased risk of future development of MetS. However, a causal involvement of cystatin C in the etiology of MetS or diabetes seems unlikely since genetic elevation of plasma cystatin C was not significantly related to incidence of these diseases.</p>}},
  author       = {{Magnusson, Martin and Molvin, John and Engström, Gunnar and Svensson, Patrik and Persson, Margaretha and Christensson, Anders and Nilsson, Peter and Melander, Olle}},
  issn         = {{1932-6203}},
  language     = {{eng}},
  month        = {{05}},
  number       = {{5}},
  publisher    = {{Public Library of Science (PLoS)}},
  series       = {{PLoS ONE}},
  title        = {{Cystatin C and risk of diabetes and the metabolic syndrome - Biomarker and genotype association analyses}},
  url          = {{http://dx.doi.org/10.1371/journal.pone.0155735}},
  doi          = {{10.1371/journal.pone.0155735}},
  volume       = {{11}},
  year         = {{2016}},
}

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Cystatin C and risk of diabetes and the metabolic syndrome - Biomarker and genotype association analyses