Chitra Iyer
Tufts Medical Center
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Publication
Featured researches published by Chitra Iyer.
Journal of Perinatology | 2013
Maria Carlota Dao; Sarbattama Sen; Chitra Iyer; David Klebenov; Simin Nikbin Meydani
Objective:To ascertain the effect of obesity-related inflammation on maternal and fetal iron status. We hypothesized that obese (Ob) pregnant women would have increased inflammation, hepcidin levels, and that their infants would have impaired iron status compared with lean (Lc) controls.Study Design:Fifteen Ob and fifteen Lc women were recruited in their second trimester of pregnancy. Markers of iron status, inflammation and hepcidin were measured in maternal and cord blood. Students t-test was used to compare Ob and Lc groups, and Pearsons correlation coefficients were determined between maternal and cord blood values.Result:Maternal C-reactive protein (P<0.01) and hepcidin (P<0.01) were higher, and cord blood iron (P<0.01) was lower in the Ob group. Maternal body mass index (P<0.01) and hepcidin (P<0.05) were negatively correlated with cord blood iron status.Conclusion:Maternal obesity is associated with impaired maternal-fetal iron transfer, potentially through hepcidin upregulation.
Journal of Perinatology | 2014
Sarbattama Sen; Chitra Iyer; Simin Nikbin Meydani
Objective:Little is known about the effect of obesity on inflammatory status in pregnant women. The objective of this study was to determine the effect of obesity on markers of inflammation, oxidative stress and micronutrient status in obese pregnant women and their infants compared with lean controls (Lc).Study Design:This was a prospective case–control study. A total of 15 obese (Ob; body mass index (BMI) >30 kg m−2) and 15 lean (BMI 18–25 kg m−2) women were recruited based on prepregnancy BMI. Vitamins A, B6, C, E and 25-hydroxyvitamin D (25(OH)D), zinc, red blood cell (RBC) folate, C-reactive protein (CRP), interleukin-6 (IL-6), tumor necrosis factor-α and oxidized and reduced glutathione were measured from maternal blood between 24 and 28 weeks of gestation. Vitamins A, B6, C and E, 25(OH)D, zinc, red blood cell folate, CRP and IL-6 were measured from cord blood at delivery.Result:Ob pregnant women have statistically significantly lower levels of vitamin B6, vitamin C, vitamin E, RBC folate, higher CRP and IL-6 levels and higher ratio of oxidized to reduced glutathione compared with Lc pregnant women. Infants born to Ob mothers did not have statistically significantly higher measures of inflammation or oxidative stress. There were no differences in micronutrient concentrations between Lc and Ob infants, but folate, vitamin B6 and zinc levels correlated strongly between mother and infant. There was no statistically significant difference in any parameter between Ob and Lc cord blood.Conclusion:Ob pregnant women have increased inflammation and oxidative stress, and lower levels of nutritional antioxidant defenses compared with Lc pregnant women. We speculate that lower antioxidant defenses combined with increased oxidative stress and inflammation may contribute to the adverse outcomes associated with pregnancy in Ob women.
American Journal of Obstetrics and Gynecology | 2013
Sarbattama Sen; Chitra Iyer; David Klebenov; Alexander Histed; Jessica Aviles; Simin Nikbin Meydani
OBJECTIVE Obese pregnancy is associated with significantly higher rates of infection, which can harm both mother and fetus. The objective of this study was to determine the impact of obesity on maternal blood immune function. STUDY DESIGN This was a cross-sectional, case control study of 15 obese (Ob) and 15 lean (Lc) subjects. Immune cell subsets, intracellular and serum cytokine production, and lymphocyte proliferation were measured in maternal blood during the second trimester of pregnancy. RESULTS Obese women had a significantly lower proportion of CD8+ and NKT cells and a higher proportion of B cells, impaired cytokine production when stimulated ex vivo, and impaired ability of lymphocytes to proliferate compared with their lean counterparts. CONCLUSION Obese pregnancy is associated with impaired cell-mediated immunity. Because perinatal infections can have serious maternal and fetal consequences, it is imperative to better understand these mechanistic underpinnings to optimize prevention and devise targeted therapy.
American Journal of Obstetrics and Gynecology | 2011
Asha Heard; Chitra Iyer; Adam Wolfberg; Jaclyn Coletta; Britta Panda; Jessica Scholl; Roa Ammari; Jeremy Kaplan; Cassandre Tanner; Michael House; Sabrina D. Craigo
American Journal of Obstetrics and Gynecology | 2011
Chitra Iyer; Asha Heard; Adam Wolfberg; Jaclyn Coletta; Britta Panda; Jessica Scholl; Roa Ammari; Jeremy Kaplan; Cassandre Tanner; Michael House; Sabrina D. Craigo
American Journal of Obstetrics and Gynecology | 2011
Jessica Scholl; Chitra Iyer; Asha Heard; Jaclyn Coletta; Britta Panda; Michelle Russell
American Journal of Obstetrics and Gynecology | 2011
Roa Ammari; Jeremy Kaplan; Adam Wolfberg; Cassandre Tanner; Chitra Iyer; Asha Heard; Jaclyn Coletta; Britta Panda; Jessica Scholl; Michael House; Sabrina D. Craigo
/data/revues/00029378/v204i1sS/S0002937810016935/ | 2011
Jessica Scholl; Chitra Iyer; Asha Heard; Jaclyn Coletta; Britta Panda; Michelle Russell
/data/revues/00029378/v204i1sS/S0002937810016522/ | 2011
Sara M. Durfee; Chitra Iyer; Asha Heard; Britta Panda; Jaclyn Coletta; Jessica Scholl; Roa Ammari; Jeremy Kaplan; Cassandre Tanner; Carol B. Benson
/data/revues/00029378/v204i1sS/S000293781001608X/ | 2011
Asha Heard; Chitra Iyer; Adam Wolfberg; Jaclyn Coletta; Britta Panda; Jessica Scholl; Roa Ammari; Jeremy Kaplan; Cassandre Tanner; Michael House; Sabrina Craigo