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Maternal homocysteine in pregnancy and offspring birthweight: epidemiological associations and Mendelian randomization analysis

Maternal homocysteine in pregnancy and offspring birthweight: epidemiological associations and Mendelian randomization analysis
Maternal homocysteine in pregnancy and offspring birthweight: epidemiological associations and Mendelian randomization analysis
Background: disturbed one-carbon (1-C) metabolism in the mother is associated with poor fetal growth but causality of this relationship has not been established.

Methods: we studied the association between maternal total homocysteine and offspring birthweight in the Pune Maternal Nutrition Study (PMNS, Pune, India) and Parthenon Cohort Study (Mysore, India). We tested for evidence of causality within a Mendelian randomization framework, using a methylenetetrahydrofolatereductase (MTHFR) gene variant rs1801133 (earlier known as 677C→T) by instrumental variable and triangulation analysis, separately and using meta-analysis.

Results: median (IQR) homocysteine concentration and mean (SD) birthweight were 8.6 µmol/l (6.7,10.8) and 2642g (379) in the PMNS and 6.0 µmol/l (5.1,7.1) and 2871g (443) in the Parthenon study. Offspring birthweight was inversely related to maternal homocysteine concentration—PMNS: –22g/SD [95% confidence interval (CI): (–50, 5), adjusted for gestational age and offspring gender]; Parthenon: –57?g (–92, –21); meta-analysis: –40g (–62, –17)]. Maternal risk genotype at rs1801133 predicted higher homocysteine concentration [PMNS: 0.30 SD/allele (0.14, 0.46); Parthenon: 0.21 SD (0.02, 0.40); meta-analysis: 0.26 SD (0.14, 0.39)]; and lower birthweight [PMNS: –46g (–102, 11, adjusted for gestational age, offspring gender and rs1801133 genotype); Parthenon: –78g (–170, 15); meta-analysis: –61g (–111, –10)]. Instrumental variable and triangulation analysis supported a causal association between maternal homocysteine concentration and offspring birthweight.

Conclusions: our findings suggest a causal role for maternal homocysteine (1-C metabolism) in fetal growth. Reducing maternal homocysteine concentrations may improve fetal growth.
maternal homocysteine, offspring birthweight, causality, MTHFR variant, folate, vitamin B12, mendelian randomization analysis
0300-5771
1487-1497
Yajnik, C.S.
ea0648f2-b384-4e5c-9e0f-45cc852e0c75
Chandak, G.R.
31769440-1e9c-4677-a8bb-ecb8ec843e73
Joglekar, C.
70e3e271-1071-46f2-9986-790d7e8fea6b
Katre, P.
8c05d156-f981-4953-a11e-afe7c3db49cf
Bhat, D.S.
75412cda-4b68-4286-82e2-8f9ea39fd842
Singh, S.N.
d7aaa488-9683-47d3-b06d-e593efa4b5da
Janipalli, C.S.
8c844d0f-d9dc-41ea-b8d8-d3abd1d47b78
Refsum, H.
e1f3bc3c-740f-4c46-b48f-68380d1b6735
Krishnaveni, G.V.
e9cc468a-8262-4dde-8eba-e047c68a3dce
Veena, S. R.
314c8753-3131-4e9a-9701-680bfdff6aee
Osmond, C.
2677bf85-494f-4a78-adf8-580e1b8acb81
Fall, C.
7171a105-34f5-4131-89d7-1aa639893b18
Yajnik, C.S.
ea0648f2-b384-4e5c-9e0f-45cc852e0c75
Chandak, G.R.
31769440-1e9c-4677-a8bb-ecb8ec843e73
Joglekar, C.
70e3e271-1071-46f2-9986-790d7e8fea6b
Katre, P.
8c05d156-f981-4953-a11e-afe7c3db49cf
Bhat, D.S.
75412cda-4b68-4286-82e2-8f9ea39fd842
Singh, S.N.
d7aaa488-9683-47d3-b06d-e593efa4b5da
Janipalli, C.S.
8c844d0f-d9dc-41ea-b8d8-d3abd1d47b78
Refsum, H.
e1f3bc3c-740f-4c46-b48f-68380d1b6735
Krishnaveni, G.V.
e9cc468a-8262-4dde-8eba-e047c68a3dce
Veena, S. R.
314c8753-3131-4e9a-9701-680bfdff6aee
Osmond, C.
2677bf85-494f-4a78-adf8-580e1b8acb81
Fall, C.
7171a105-34f5-4131-89d7-1aa639893b18

Yajnik, C.S., Chandak, G.R., Joglekar, C., Katre, P., Bhat, D.S., Singh, S.N., Janipalli, C.S., Refsum, H., Krishnaveni, G.V., Veena, S. R., Osmond, C. and Fall, C. (2014) Maternal homocysteine in pregnancy and offspring birthweight: epidemiological associations and Mendelian randomization analysis. International Journal of Epidemiology, 43 (5), 1487-1497. (doi:10.1093/ije/dyu132). (PMID:25052622)

Record type: Article

Abstract

Background: disturbed one-carbon (1-C) metabolism in the mother is associated with poor fetal growth but causality of this relationship has not been established.

Methods: we studied the association between maternal total homocysteine and offspring birthweight in the Pune Maternal Nutrition Study (PMNS, Pune, India) and Parthenon Cohort Study (Mysore, India). We tested for evidence of causality within a Mendelian randomization framework, using a methylenetetrahydrofolatereductase (MTHFR) gene variant rs1801133 (earlier known as 677C→T) by instrumental variable and triangulation analysis, separately and using meta-analysis.

Results: median (IQR) homocysteine concentration and mean (SD) birthweight were 8.6 µmol/l (6.7,10.8) and 2642g (379) in the PMNS and 6.0 µmol/l (5.1,7.1) and 2871g (443) in the Parthenon study. Offspring birthweight was inversely related to maternal homocysteine concentration—PMNS: –22g/SD [95% confidence interval (CI): (–50, 5), adjusted for gestational age and offspring gender]; Parthenon: –57?g (–92, –21); meta-analysis: –40g (–62, –17)]. Maternal risk genotype at rs1801133 predicted higher homocysteine concentration [PMNS: 0.30 SD/allele (0.14, 0.46); Parthenon: 0.21 SD (0.02, 0.40); meta-analysis: 0.26 SD (0.14, 0.39)]; and lower birthweight [PMNS: –46g (–102, 11, adjusted for gestational age, offspring gender and rs1801133 genotype); Parthenon: –78g (–170, 15); meta-analysis: –61g (–111, –10)]. Instrumental variable and triangulation analysis supported a causal association between maternal homocysteine concentration and offspring birthweight.

Conclusions: our findings suggest a causal role for maternal homocysteine (1-C metabolism) in fetal growth. Reducing maternal homocysteine concentrations may improve fetal growth.

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More information

e-pub ahead of print date: 21 July 2014
Published date: 1 October 2014
Keywords: maternal homocysteine, offspring birthweight, causality, MTHFR variant, folate, vitamin B12, mendelian randomization analysis
Organisations: Human Development & Health

Identifiers

Local EPrints ID: 375454
URI: http://eprints.soton.ac.uk/id/eprint/375454
DOI: doi:10.1093/ije/dyu132
ISSN: 0300-5771
PURE UUID: cfb737df-43ff-419c-b8fd-298f6ee42766
ORCID for C. Osmond: ORCID iD orcid.org/0000-0002-9054-4655
ORCID for C. Fall: ORCID iD orcid.org/0000-0003-4402-5552

Catalogue record

Date deposited: 26 Mar 2015 14:31
Last modified: 15 Mar 2024 02:50

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Contributors

Author: C.S. Yajnik
Author: G.R. Chandak
Author: C. Joglekar
Author: P. Katre
Author: D.S. Bhat
Author: S.N. Singh
Author: C.S. Janipalli
Author: H. Refsum
Author: G.V. Krishnaveni
Author: S. R. Veena
Author: C. Osmond ORCID iD
Author: C. Fall ORCID iD

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