Underweight Full-Term Indian Neonates Show Differences in Umbilical Cord Blood Leukocyte Phenotype: A Cross-Sectional Study

Rathore, Deepak Kumar; Nair, Deepa; Raza, Saimah; Saini, Sharanjot; Singh, Reeta; Kumar, Ashutosh; Tripathi, Reva; Ramji, Siddarth; Batra, Aruna; Aggarwal, Kailash Chandra; Chellani, Harish; Arya, Sugandha; Bhatla, Neerja; Paul, Vinod K.; Aggarwal, Rashmi; Agarwal, Nidhi; Umesh, M. H.; Sopory, Shailaja; Natchu, Uma Chandra Mouli; Bhatnagar, Shinjini; Bal, Vineeta; Rath, Satyajit; Wadhwa, Nitya

doi:10.1371/journal.pone.0123589

Cited by 9 publications

(8 citation statements)

References 62 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…On the other hand, siblings were far similar to each other in memory subset frequencies than non-siblings were, suggesting a hereditary component or shared environmental factors in regulating memory lymphocyte frequencies. Any similarity between siblings could be attributed to early life influences, since it is well recognized that both intra-uterine [49,50] and neonatal [51] stress impacts immune system development, and a recent study [13] has shown a prominent role for co-habitation in determining immune phenotypes. Our findings are consistent with two previous studies [1,14] which report high degree of heritability for majority of immune subsets.…”

Section: Discussionmentioning

confidence: 99%

Cell-intrinsic regulation of peripheral memory-phenotype T cell frequencies

et al. 2018

Self Cite

View full text Add to dashboard Cite

Memory T and B lymphocyte numbers are thought to be regulated by recent and cumulative microbial exposures. We report here that memory-phenotype lymphocyte frequencies in B, CD4 and CD8 T-cells in 3-monthly serial bleeds from healthy young adult humans were relatively stable over a 1-year period, while Plasmablast frequencies were not, suggesting that recent environmental exposures affected steady state levels of recently activated but not of memory lymphocyte subsets. Frequencies of memory B and CD4 T cells were not correlated, suggesting that variation in them was unlikely to be determined by cumulative antigenic exposures. Immunophenotyping of adult siblings showed high concordance in memory, but not of recently activated lymphocyte subsets. To explore the possibility of cell-intrinsic regulation of T cell memory, we screened effector memory-phenotype T cell (TEM) frequencies in common independent inbred mice strains. Using two pairs from these strains that differed predominantly in either CD4 TEM and/or CD8 TEM frequencies, we constructed bi-parental bone marrow chimeras in F1 recipient mice, and found that memory T cell frequencies in recipient mice were determined by donor genotypes. Together, these data suggest cell-autonomous determination of memory T niche size, and suggest mechanisms maintaining immune variability.

show abstract

Section: Discussionmentioning

confidence: 99%

Cell-intrinsic regulation of peripheral memory-phenotype T cell frequencies

et al. 2018

Self Cite

View full text Add to dashboard Cite

show abstract

“…In healthy adult individuals, the frequency of classical monocytes varies from 80 to 90% of total monocytes. On the other hand, nonclassical monocytes constitute about 8-10%, whereas neonates have a low number of nonclassical monocytes [8, 9]. The phenotype and function of monocyte subsets change extensively in inflammatory disease conditions.…”

Section: Introductionmentioning

confidence: 99%

Absence of Nonclassical Monocytes in Hemolytic Patients: Free Hb and NO-Mediated Mechanism

Singhal

Rathore

Bhakuni

et al. 2019

Journal of Immunology Research

Self Cite

View full text Add to dashboard Cite

In a recent work, we have described the kinetics among the monocyte subsets in the peripheral blood of hemolytic patients including paroxysmal nocturnal hemoglobinuria (PNH) and sickle cell disease (SCD). After engulfing Hb-activated platelets, classical monocytes (CD14+CD16-) significantly transformed into highly inflammatory (CD14+CD16hi) subsets in vitro. An estimated 40% of total circulating monocytes in PNH and 70% in SCD patients existed as CD14+CD16hi subsets. In this study, we show that the nonclassical (CD14dimCD16+) monocyte subsets are nearly absent in patients with PNH or SCD, compared to 10-12% cells in healthy individuals. In mechanism, we have described the unique role of both free Hb and nitric oxide (NO) in reducing number of nonclassical subsets more than classical monocytes. After engulfing Hb-activated platelets, the monocytes including nonclassical subsets acquired rapid cell death within 12 h in vitro. Further, the treatment to monocytes either with the secretome of Hb-activated platelets containing NO and free Hb or purified free Hb along with GSNO (a physiological NO donor) enhanced rapid cell death. Besides, our data from both PNH and SCD patients exhibited a direct correlation between intracellular NO and cell death marker 7AAD in monocytes from the peripheral blood. Our data together suggest that due to the immune surveillance nature, the nonclassical or patrolling monocytes are encountered frequently by Hb-activated platelets, free Hb, and NO in the circulation of hemolytic patients and are predisposed to die rapidly.

show abstract

“…In accordance with this hypothesis, an increased risk of infections and aberrant immune development has been reported in both preterm [ 14 26 ] and SGA infants [ 27 28 29 30 ].…”

Section: Discussionmentioning

confidence: 71%

Birth Weight and the Development of Functional Gastrointestinal Disorders in Infants

Martire

Mauro

Salvatore

et al. 2020

Pediatr Gastroenterol Hepatol Nutr

View full text Add to dashboard Cite

Purpose To assess the association between birth weight and the development of functional gastrointestinal disorders (FGIDs) in the first year of life. Methods This is a secondary analysis of a prospective cohort multicenter study including neonates, consecutively enrolled at birth, and followed up for one year. At birth all infants were classified by birth weight as extremely low (ELBW), very low, or low when <1,000, <1,500, and <2,500 g, respectively, and by birth weight for gestational age as appropriate (AGA, weight in the 10–90th percentile), small (SGA, weight <10th percentile), and large (LGA, weight >90th percentile) for gestational age. FGIDs were classified according to the Rome III criteria and assessed at 1, 3, 6, and 12 months of life. Results Among 1,152 newborns enrolled, 934 (81.1%) completed the study: 302 (32.3%) were preterm, 35 (3.7%) were ELBW, 104 (11.1%) were SGA, 782 (83.7%) were AGA, and 48 (5.1%) were LGA infants. Overall, throughout the first year of life, 718 (76.9%) reported at least one FGID. The proportion of infants presenting with at least one FGID was significantly higher in ELBW (97%) compared to LBW (74%) ( p =0.01) and in LGA (85.4%) and SGA (85.6%) compared to AGA (75.2%) ( p =0.0001). On multivariate analysis, SGA was significantly associated with infantile colic. Conclusion We observed an increased risk of FGIDs in ELBW, SGA, and LGA neonates. Our results suggest that prenatal factors determining birth weight may influence the development of FGIDs in infants. Understanding the role of all potential risk factors may provide new insights and targeted approaches for FGIDs.

show abstract

Underweight Full-Term Indian Neonates Show Differences in Umbilical Cord Blood Leukocyte Phenotype: A Cross-Sectional Study

Cited by 9 publications

References 62 publications

Cell-intrinsic regulation of peripheral memory-phenotype T cell frequencies

Cell-intrinsic regulation of peripheral memory-phenotype T cell frequencies

Absence of Nonclassical Monocytes in Hemolytic Patients: Free Hb and NO-Mediated Mechanism

Birth Weight and the Development of Functional Gastrointestinal Disorders in Infants

Contact Info

Product

Resources

About