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A Study of Adenylate Kinase Locus 1 (Ak(1)) Genetic Polymorphism in Diabetic Pregnancy

BACKGROUND: Previous studies suggest that adenylate kinase locus 1 (Ak(1)) has an important role in the control of blood glucose level and in the glycation of structural and functional proteins in type 2 diabetes and in the balanced development of feto-placental unit in healthy puerperae (HP). In th...

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Autores principales: Gloria-Bottini, Fulvia, Pietropolli, Adalgisa, Neri, Anna, Coppeta, Luca, Magrini, Andrea, Bottini, Egidio
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Avicenna Research Institute 2014
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Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4138424/
https://www.ncbi.nlm.nih.gov/pubmed/25202675
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author Gloria-Bottini, Fulvia
Pietropolli, Adalgisa
Neri, Anna
Coppeta, Luca
Magrini, Andrea
Bottini, Egidio
author_facet Gloria-Bottini, Fulvia
Pietropolli, Adalgisa
Neri, Anna
Coppeta, Luca
Magrini, Andrea
Bottini, Egidio
author_sort Gloria-Bottini, Fulvia
collection PubMed
description BACKGROUND: Previous studies suggest that adenylate kinase locus 1 (Ak(1)) has an important role in the control of blood glucose level and in the glycation of structural and functional proteins in type 2 diabetes and in the balanced development of feto-placental unit in healthy puerperae (HP). In this study, an attempt was made to investigate the relationship of Ak(1) with maternal and neonatal parameters in puerperae with gestational diabetes (GDP) and with preexisting type 1 diabetes (T1DP). METHODS: This study was carried on 402 HP, 347 consecutive healthy newborns, 102 GDP and 111 T1DP with their newborn infants. Ak(1) phenotype was determined by starch gel electrophoresis. Chi-square test of independence was carried out by SPSS program. The analysis of three way contingency table was carried out by a loglinear model. Significant level was 0.05. RESULTS: In T1DP, the frequency of Ak(1)*2 allele was higher than in GDP and in HP. Serum glucose level was higher in T1DP than in GDP with higher values in carriers of Ak(1)*2 allele. Neonatal hypoglycemia was more frequent in T1DP than in GDP with a positive association with Ak(1)*2 allele. The correlation between birth weight (BW) and placental weight (PW) was lower in infants from T1DP than HP. In healthy puerperae the correlation is higher in Ak(1) 2-1 than in Ak(1)1 phenotype while in diabetic puerperae the pattern is reversed with lower values in Ak(1)2-1 than in Ak(1)1 phenotype. The lowest value of correlation is observed in infants from T1D mothers carrying the Ak(1)*2 allele. CONCLUSION: The data confirmed the involvement of Ak(1) in glucose metabolism and showed a disturbance of the balance between placental and fetal growth which was more marked in T1DP.
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spelling pubmed-41384242014-09-08 A Study of Adenylate Kinase Locus 1 (Ak(1)) Genetic Polymorphism in Diabetic Pregnancy Gloria-Bottini, Fulvia Pietropolli, Adalgisa Neri, Anna Coppeta, Luca Magrini, Andrea Bottini, Egidio J Reprod Infertil Short Communication BACKGROUND: Previous studies suggest that adenylate kinase locus 1 (Ak(1)) has an important role in the control of blood glucose level and in the glycation of structural and functional proteins in type 2 diabetes and in the balanced development of feto-placental unit in healthy puerperae (HP). In this study, an attempt was made to investigate the relationship of Ak(1) with maternal and neonatal parameters in puerperae with gestational diabetes (GDP) and with preexisting type 1 diabetes (T1DP). METHODS: This study was carried on 402 HP, 347 consecutive healthy newborns, 102 GDP and 111 T1DP with their newborn infants. Ak(1) phenotype was determined by starch gel electrophoresis. Chi-square test of independence was carried out by SPSS program. The analysis of three way contingency table was carried out by a loglinear model. Significant level was 0.05. RESULTS: In T1DP, the frequency of Ak(1)*2 allele was higher than in GDP and in HP. Serum glucose level was higher in T1DP than in GDP with higher values in carriers of Ak(1)*2 allele. Neonatal hypoglycemia was more frequent in T1DP than in GDP with a positive association with Ak(1)*2 allele. The correlation between birth weight (BW) and placental weight (PW) was lower in infants from T1DP than HP. In healthy puerperae the correlation is higher in Ak(1) 2-1 than in Ak(1)1 phenotype while in diabetic puerperae the pattern is reversed with lower values in Ak(1)2-1 than in Ak(1)1 phenotype. The lowest value of correlation is observed in infants from T1D mothers carrying the Ak(1)*2 allele. CONCLUSION: The data confirmed the involvement of Ak(1) in glucose metabolism and showed a disturbance of the balance between placental and fetal growth which was more marked in T1DP. Avicenna Research Institute 2014 /pmc/articles/PMC4138424/ /pubmed/25202675 Text en Copyright © 2014 Avicenna Research Institute http://creativecommons.org/licenses/by-nc/3.0/ This work is licensed under a Creative Commons Attribution-NonCommercial 3.0 Unported License which allows users to read, copy, distribute and make derivative works for non-commercial purposes from the material, as long as the author of the original work is cited properly.
spellingShingle Short Communication
Gloria-Bottini, Fulvia
Pietropolli, Adalgisa
Neri, Anna
Coppeta, Luca
Magrini, Andrea
Bottini, Egidio
A Study of Adenylate Kinase Locus 1 (Ak(1)) Genetic Polymorphism in Diabetic Pregnancy
title A Study of Adenylate Kinase Locus 1 (Ak(1)) Genetic Polymorphism in Diabetic Pregnancy
title_full A Study of Adenylate Kinase Locus 1 (Ak(1)) Genetic Polymorphism in Diabetic Pregnancy
title_fullStr A Study of Adenylate Kinase Locus 1 (Ak(1)) Genetic Polymorphism in Diabetic Pregnancy
title_full_unstemmed A Study of Adenylate Kinase Locus 1 (Ak(1)) Genetic Polymorphism in Diabetic Pregnancy
title_short A Study of Adenylate Kinase Locus 1 (Ak(1)) Genetic Polymorphism in Diabetic Pregnancy
title_sort study of adenylate kinase locus 1 (ak(1)) genetic polymorphism in diabetic pregnancy
topic Short Communication
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4138424/
https://www.ncbi.nlm.nih.gov/pubmed/25202675
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