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Dive into the research topics where S V Gandhi is active.

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Featured researches published by S V Gandhi.


Trials | 2012

MAVIDOS Maternal Vitamin D Osteoporosis Study: study protocol for a randomized controlled trial. The MAVIDOS Study Group

Nicholas C. Harvey; Kassim Javaid; Nick Bishop; Stephen Kennedy; A T Papageorghiou; Robert Fraser; S V Gandhi; Inez Schoenmakers; Ann Prentice; C Cooper

MAVIDOS is a randomised, double-blind, placebo-controlled trial (ISRCTN82927713, registered 2008 Apr 11), funded by Arthritis Research UK, MRC, Bupa Foundation and NIHR.BackgroundOsteoporosis is a major public health problem as a result of associated fragility fractures. Skeletal strength increases from birth to a peak in early adulthood. This peak predicts osteoporosis risk in later life. Vitamin D insufficiency in pregnancy is common (31% in a recent Southampton cohort) and predicts reduced bone mass in the offspring. In this study we aim to test whether offspring of mothers supplemented with vitamin D in pregnancy have higher bone mass at birth than those whose mothers were not supplemented.Methods/DesignWomen have their vitamin D status assessed after ultrasound scanning in the twelfth week of pregnancy at 3 trial centres (Southampton, Sheffield, Oxford). Women with circulating 25(OH)-vitamin D levels 25-100 nmol/l are randomised in a double-blind design to either oral vitamin D supplement (1000 IU cholecalciferol/day, n = 477) or placebo at 14 weeks (n = 477). Questionnaire data include parity, sunlight exposure, dietary information, and cigarette and alcohol consumption. At 19 and 34 weeks maternal anthropometry is assessed and blood samples taken to measure 25(OH)-vitamin D, PTH and biochemistry. At delivery venous umbilical cord blood is collected, together with umbilical cord and placental tissue. The babies undergo DXA assessment of bone mass within the first 14 days after birth, with the primary outcome being whole body bone mineral content adjusted for gestational age and age. Children are then followed up with yearly assessment of health, diet, physical activity and anthropometric measures, with repeat assessment of bone mass by DXA at age 4 years.DiscussionAs far as we are aware, this randomised trial is one of the first ever tests of the early life origins hypothesis in human participants and has the potential to inform public health policy regarding vitamin D supplementation in pregnancy. It will also provide a valuable resource in which to study the influence of maternal vitamin D status on other childhood outcomes such as glucose tolerance, blood pressure, cardiovascular function, IQ and immunology.


Biomedical Engineering Online | 2006

Comparison of human uterine cervical electrical impedance measurements derived using two tetrapolar probes of different sizes

S V Gandhi; Dawn Walker; Brian H Brown; Dilly Anumba

BackgroundWe sought to compare uterine cervical electrical impedance spectroscopy measurements employing two probes of different sizes, and to employ a finite element model to predict and compare the fraction of electrical current derived from subepithelial stromal tissue.MethodsCervical impedance was measured in 12 subjects during early pregnancy using 2 different sizes of the probes on each subject.ResultsMean cervical resistivity was significantly higher (5.4 vs. 2.8 Ωm; p < 0.001) with the smaller probe in the frequency rage of 4–819 kHz. There was no difference in the short-term intra-observer variability between the two probes. The cervical impedance measurements derived in vivo followed the pattern predicted by the finite element model.ConclusionInter-electrode distance on the probes for measuring cervical impedance influences the tissue resistivity values obtained. Determining the appropriate probe size is necessary when conducting clinical studies of resistivity of the cervix and other human tissues.


Clinical Dysmorphology | 2008

Fetal megalourethra associated with hypoplastic left heart and imperforate anus: a previously unreported association.

S V Gandhi; Marta C. Cohen; Alan Sprigg; Lawrence Roberts; Dilly Anumba

We report two cases of a fetus with a megalourethra associated with a hypoplastic left heart, dilated and echogenic bowels, vesico-colonic fistula and an imperforate anus. This combination of fetal abnormalities may represent an unclassified syndrome.


Journal of Bone and Mineral Research | 2018

Gestational vitamin D supplementation leads to reduced perinatal RXRA DNA methylation: Results from the MAVIDOS trial

Elizabeth M. Curtis; Nevena Krstic; Eloise Cook; S D'Angelo; Sarah Crozier; Rebecca Moon; Robert Murray; Emma Garratt; Paula Costello; Jane K. Cleal; Brogan Ashley; Nick Bishop; Stephen Kennedy; A T Papageorghiou; Inez Schoenmakers; Robert Fraser; S V Gandhi; Ann Prentice; M Kassim Javaid; Hazel Inskip; Keith M. Godfrey; Christopher G. Bell; Karen A. Lillycrop; C Cooper; Nicholas C. Harvey

We have previously demonstrated inverse associations between maternal 25(OH)‐vitamin D status and perinatal DNA methylation at the retinoid‐X‐receptor‐alpha (RXRA) locus and between RXRA methylation and offspring bone mass. In this study, we used an existing randomized trial to test the hypothesis that maternal gestational vitamin D supplementation would lead to reduced perinatal RXRA locus DNA methylation. The Maternal Vitamin D Osteoporosis Study (MAVIDOS) was a multicenter, double‐blind, randomized, placebo‐controlled trial of 1000 IU/day cholecalciferol or matched placebo from 14 weeks’ gestation until delivery. Umbilical cord (fetal) tissue was collected at birth and frozen at −80°C (n = 453). Pyrosequencing was used to undertake DNA methylation analysis at 10 CpG sites within the RXRA locus (identified previously). T tests were used to assess differences between treatment groups in methylation at the three most representative CpG sites. Overall, methylation levels were significantly lower in the umbilical cord from offspring of cholecalciferol‐supplemented mothers, reaching statistical significance at four CpG sites, represented by CpG5: mean difference in % methylation between the supplemented and placebo groups was −1.98% (95% CI, −3.65 to −0.32, p = 0.02). ENCODE (Encyclopedia of DNA Elements) evidence supports the functionality of this locus with strong DNase hypersensitivity and enhancer chromatin within biologically relevant cell types including osteoblasts. Enrichment of the enhancer‐related H3K4me1 histone mark is also seen in this region, as are binding sites for a range of transcription factors with roles in cell proliferation, response to stress, and growth factors. Our findings are consistent with previous observational results and provide new evidence that maternal gestational supplementation with cholecalciferol leads to altered perinatal epigenetic marking, informing mechanistic understanding of early life mechanisms related to maternal vitamin D status, epigenetic marks, and bone development.


The Lancet Diabetes & Endocrinology | 2016

Maternal gestational vitamin D supplementation and offspring bone health (MAVIDOS): a multicentre, double-blind, randomised placebo-controlled trial

C Cooper; N C Harvey; Nick Bishop; Stephen Kennedy; A T Papageorghiou; Inez Schoenmakers; Robert Fraser; S V Gandhi; A J Carr; S D'Angelo; Sarah Crozier; Rebecca Moon; N K Arden; Elaine M. Dennison; Keith M. Godfrey; Hazel Inskip; Ann Prentice; M Z Mughal; Richard Eastell; David M. Reid; M K Javaid


European Journal of Obstetrics & Gynecology and Reproductive Biology | 2006

Electrical impedance spectroscopy of the cervix in non-pregnant and pregnant women

S V Gandhi; Dawn Walker; Pete Milnes; Soma Mukherjee; Brian H Brown; Dilly Anumba


The Journal of Clinical Endocrinology and Metabolism | 2016

Determinants of the Maternal 25-Hydroxyvitamin D Response to Vitamin D Supplementation During Pregnancy

Rebecca Moon; Nicholas C. Harvey; C Cooper; S D'Angelo; Sarah Crozier; Hazel Inskip; Inez Schoenmakers; A Prentice; N K Arden; Nick Bishop; A J Carr; Elaine M. Dennison; Richard Eastell; Robert Fraser; S V Gandhi; Keith M. Godfrey; Stephen Kennedy; M Z Mughal; A T Papageorghiou; David M. Reid; Sian Robinson; M K Javaid


Rheumatology | 2017

PERINATAL DNA METHYLATION AT THE RXRA PROMOTER IS ASSOCIATED WITH GESTATIONAL VITAMIN D SUPPLEMENTATION: RESULTS FROM THE MAVIDOS TRIAL

Eloise Cook; Elizabeth M. Curtis; Nevena Krstic; S D'Angelo; Sarah Crozier; Rebecca Moon; Robert Murray; Emma Garratt; Paula Costello; Nick Bishop; S Kennedy; A T Papageorghiou; Inez Schoenmakers; Robert Fraser; S V Gandhi; A Prentice; M K Javaid; Hazel Inskip; Keith M. Godfrey; Christopher G. Bell; C Cooper; Karen A. Lillycrop; N C Harvey; Grp Mavidost.


Osteoporosis International | 2018

PLASMA CTX IN PREGNANCY IS ALTERED BY CHOLECALCIFEROL SUPPLEMENTATION AND IS ASSOCIATED WITH MATERNAL BONE INDICES: THE MAVIDOS TRIAL

Elizabeth M. Curtis; K Maslin; S D'Angelo; Rebecca Moon; Sarah Crozier; F Gossiel; Nick Bishop; S Kennedy; A T Papageorghiou; Robert Fraser; S V Gandhi; A Prentice; Hazel Inskip; Keith M. Godfrey; Inez Schoenmakers; M K Javaid; Richard Eastell; C Cooper; N C Harvey


Rheumatology | 2017

157. PERINATAL DNA METHYLATION AT THE RXRA PROMOTER IS ASSOCIATED WITH GESTATIONAL VITAMIN D SUPPLEMENTATION: RESULTS FROM THE MAVIDOS TRIAL

Eloise Cook; Elizabeth M. Curtis; Nevena Krstic; S D'Angelo; Sarah Crozier; Rebecca Moon; Robert Murray; Emma Garratt; Paula Costello; Nick Bishop; Stephen Kennedy; A T Papageorghiou; Inez Schoenmakers; R. Fraser; S V Gandhi; Ann Prentice; M Kassim Javaid; Hazel Inskip; Keith M. Godfrey; Christopher G. Bell; C Cooper; Karen A. Lillycrop; Nicholas C. Harvey

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C Cooper

Southampton General Hospital

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Nick Bishop

University of Sheffield

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Rebecca Moon

University of Southampton

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Sarah Crozier

University of Southampton

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Hazel Inskip

University Hospital Southampton NHS Foundation Trust

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S D'Angelo

University of Southampton

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Keith M. Godfrey

University Hospital Southampton NHS Foundation Trust

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