Satyajeet P Khare, Ayush Madhok, Indumathi Patta, Krishna K Sukla, Vipul V Wagh, Pooja S Kunte, Deepa Raut, Dattatray Bhat, Kalyanaraman Kumaran, Caroline Fall, Utpal Tatu, Giriraj R Chandak, Chittaranjan S Yajnik, Sanjeev Galande
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The interventions included: (1) vitamin B12+multi-micronutrients as per the United Nations International Multiple Micronutrient Antenatal Preparation, and proteins (B12+MMN), (2) vitamin B12 (B12 alone), and (3) placebo. Intervention improved maternal pre-conceptional and in-pregnancy micronutrient nutrition. Gene expression analysis in cord blood mononuclear cells in 88 pregnancies revealed 75 differentially expressed genes between the B12+MMN and placebo groups. The enriched biological processes included G2/M phase transition, chromosome segregation, and nuclear division. Enriched pathways included, mitotic spindle checkpoint and DNA damage response while enriched human phenotypes were sloping forehead and decreased head circumference. Fructose-bisphosphatase 2 (<i>FBP2)</i> and Cell Division Cycle Associated 2 (<i>CDCA2)</i> genes were under-expressed in the B12 alone group. The latter, involved in chromosome segregation was under-expressed in both intervention groups. Based on the role of B-complex vitamins in the synthesis of nucleotides and S-adenosyl methionine, and the roles of vitamins A and D on gene expression, we propose that the multi-micronutrient intervention epigenetically affected cell cycle dynamics. Neonates in the B12+MMN group had the highest ponderal index. Follow-up studies will reveal if the intervention and the altered biological processes influence offspring diabesity.</p>","PeriodicalId":49167,"journal":{"name":"Journal of Developmental Origins of Health and Disease","volume":"14 3","pages":"437-448"},"PeriodicalIF":1.8000,"publicationDate":"2023-06-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Differential expression of genes influencing mitotic processes in cord blood mononuclear cells after a pre-conceptional micronutrient-based randomised controlled trial: Pune Rural Intervention in Young Adolescents (PRIYA).\",\"authors\":\"Satyajeet P Khare, Ayush Madhok, Indumathi Patta, Krishna K Sukla, Vipul V Wagh, Pooja S Kunte, Deepa Raut, Dattatray Bhat, Kalyanaraman Kumaran, Caroline Fall, Utpal Tatu, Giriraj R Chandak, Chittaranjan S Yajnik, Sanjeev Galande\",\"doi\":\"10.1017/S204017442200068X\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>In The Pune Maternal Nutrition Study, vitamin B12 deficiency was seen in 65% of pregnant women, folate deficiency was rare. 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引用次数: 0
摘要
在普纳孕产妇营养研究中,65% 的孕妇缺乏维生素 B12,叶酸缺乏的情况很少见。母体总同型半胱氨酸浓度与后代出生体重成反比,低维生素 B12 浓度和高叶酸浓度预示着后代脂肪含量和胰岛素抵抗力较高。这些发现为 "普纳农村青少年干预 "孕前随机对照试验提供了指导。干预措施包括(1) 根据联合国国际多种微量营养素产前准备方案提供的维生素 B12+ 多种微量营养素和蛋白质(B12+MMN),(2) 维生素 B12(仅提供 B12),以及 (3) 安慰剂。干预措施改善了孕产妇的孕前和孕期微量营养素营养状况。对 88 名孕妇的脐带血单核细胞进行基因表达分析后发现,B12+MMN 组和安慰剂组之间有 75 个基因表达不同。富集的生物过程包括 G2/M 期转变、染色体分离和核分裂。富集的途径包括有丝分裂纺锤体检查点和 DNA 损伤反应,而富集的人类表型是前额倾斜和头围减小。果糖二磷酸酶 2(FBP2)和细胞分裂周期相关 2(CDCA2)基因在单用 B12 组中表达不足。参与染色体分离的 CDCA2 基因在两个干预组中都表达不足。根据复合维生素 B 在核苷酸和 S-腺苷蛋氨酸合成中的作用,以及维生素 A 和 D 在基因表达中的作用,我们认为多种微量营养素干预措施对细胞周期动力学产生了表观遗传学影响。B12+MMN组的新生儿思索指数最高。后续研究将揭示干预和生物过程的改变是否会影响后代的肥胖。
Differential expression of genes influencing mitotic processes in cord blood mononuclear cells after a pre-conceptional micronutrient-based randomised controlled trial: Pune Rural Intervention in Young Adolescents (PRIYA).
In The Pune Maternal Nutrition Study, vitamin B12 deficiency was seen in 65% of pregnant women, folate deficiency was rare. Maternal total homocysteine concentrations were inversely associated with offspring birthweight, and low vitamin B12 and high folate concentrations predicted higher offspring adiposity and insulin resistance. These findings guided a nested pre-conceptional randomised controlled trial 'Pune Rural Intervention in Young Adolescents'. The interventions included: (1) vitamin B12+multi-micronutrients as per the United Nations International Multiple Micronutrient Antenatal Preparation, and proteins (B12+MMN), (2) vitamin B12 (B12 alone), and (3) placebo. Intervention improved maternal pre-conceptional and in-pregnancy micronutrient nutrition. Gene expression analysis in cord blood mononuclear cells in 88 pregnancies revealed 75 differentially expressed genes between the B12+MMN and placebo groups. The enriched biological processes included G2/M phase transition, chromosome segregation, and nuclear division. Enriched pathways included, mitotic spindle checkpoint and DNA damage response while enriched human phenotypes were sloping forehead and decreased head circumference. Fructose-bisphosphatase 2 (FBP2) and Cell Division Cycle Associated 2 (CDCA2) genes were under-expressed in the B12 alone group. The latter, involved in chromosome segregation was under-expressed in both intervention groups. Based on the role of B-complex vitamins in the synthesis of nucleotides and S-adenosyl methionine, and the roles of vitamins A and D on gene expression, we propose that the multi-micronutrient intervention epigenetically affected cell cycle dynamics. Neonates in the B12+MMN group had the highest ponderal index. Follow-up studies will reveal if the intervention and the altered biological processes influence offspring diabesity.
期刊介绍:
JDOHaD publishes leading research in the field of Developmental Origins of Health and Disease (DOHaD). The Journal focuses on the environment during early pre-natal and post-natal animal and human development, interactions between environmental and genetic factors, including environmental toxicants, and their influence on health and disease risk throughout the lifespan. JDOHaD publishes work on developmental programming, fetal and neonatal biology and physiology, early life nutrition, especially during the first 1,000 days of life, human ecology and evolution and Gene-Environment Interactions.
JDOHaD also accepts manuscripts that address the social determinants or education of health and disease risk as they relate to the early life period, as well as the economic and health care costs of a poor start to life. Accordingly, JDOHaD is multi-disciplinary, with contributions from basic scientists working in the fields of physiology, biochemistry and nutrition, endocrinology and metabolism, developmental biology, molecular biology/ epigenetics, human biology/ anthropology, and evolutionary developmental biology. Moreover clinicians, nutritionists, epidemiologists, social scientists, economists, public health specialists and policy makers are very welcome to submit manuscripts.
The journal includes original research articles, short communications and reviews, and has regular themed issues, with guest editors; it is also a platform for conference/workshop reports, and for opinion, comment and interaction.