Please use this identifier to cite or link to this item: http://hdl.handle.net/123456789/605
Title: Underweight full-term Indian neonates show differences in umbilical cord blood leukocyte phenotype: a cross-sectional study
Authors: Wadhwa, Nitya
Rathore, Deepak K
Nair, Deepa
Raza, Saimah
Saini, Savita
Singh, Reeta
Kumar, Amit
Tripathi, Reva
Ramji, Siddarth
Batra, Aruna
Aggarwal, Kailash C
Chellani, Harish K
Arya, Sugandha
Bhatla, Neerja
Paul, Vinod K
Aggarwal, Ramesh
Agarwal, Nidhi
Mehta, Umesh
Sopory, Shailaja
Natchu, Uma Chandra Mouli
Bhatnagar, Shinjini
Bal, Vineeta
Rath, Satyajit
Issue Date: Apr-2015
Publisher: PLOS
Abstract: BACKGROUND: While infections are a major cause of neonatal mortality in India even in full-term neonates, this is an especial problem in the large proportion (~20%) of neonates born underweight (or small-for-gestational-age; SGA). One potential contributory factor for this susceptibility is the possibility that immune system maturation may be affected along with intrauterine growth retardation. METHODS: In order to examine the possibility that differences in immune status may underlie the susceptibility of SGA neonates to infections, we enumerated the frequencies and concentrations of 22 leukocyte subset populations as well as IgM and IgA levels in umbilical cord blood from full-term SGA neonates and compared them with values from normal-weight (or appropriate-for-gestational-age; AGA) full-term neonates. We eliminated most SGA-associated risk factors in the exclusion criteria so as to ensure that AGA-SGA differences, if any, would be more likely to be associated with the underweight status itself. RESULTS: An analysis of 502 such samples, including 50 from SGA neonates, showed that SGA neonates have significantly fewer plasmacytoid dendritic cells (pDCs), a higher myeloid DC (mDC) to pDC ratio, more natural killer (NK) cells, and higher IgM levels in cord blood in comparison with AGA neonates. Other differences were also observed such as tendencies to lower CD4:CD8 ratios and greater prominence of inflammatory monocytes, mDCs and neutrophils, but while some of them had substantial differences, they did not quite reach the standard level of statistical significance. CONCLUSIONS: These differences in cellular lineages of the immune system possibly reflect stress responses in utero associated with growth restriction. Increased susceptibility to infections may thus be linked to complex immune system dysregulation rather than simply retarded immune system maturation.
URI: http://hdl.handle.net/123456789/605
Appears in Collections:Immumo Biology- I, Publications

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