Literature DB >> 30464858

Use of Mannose-Binding Lectin Gene Polymorphisms and the Serum MBL Level for the Early Detection of Neonatal Sepsis.

Magda Badawy1, Dalia S Mosallam1, Doaa Saber1, Hanan Madani2.   

Abstract

Background  Mannose-binding lectin (MBL) is a component of innate immunity and is particularly important in neonates, in whom adaptive immunity has not yet completely developed. MBL deficiency and MBL2 gene polymorphisms are associated with an opsonization defect and have been associated with neonatal sepsis. Aim  The aim of our study was to assess serum MBL levels and genotype MBL2 genes to determine whether they can serve as markers for predicting neonatal sepsis in neonatal intensive care units. Patients and Methods  A case-control study was conducted with 114 neonates classified into two groups: the septic group included 64 neonates (41 preterm and 23 full-term infants), and the non-septic control group included 50 neonates (29 preterm and 21 full-term infants). Polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) analysis was used to genotype MBL2 gene exon 1 (rs1800450) and (rs1800451) SNPs. Enzyme-linked immunosorbent assay (ELISA) was used to measure MBL serum concentrations. Results  The polymorphic genotypes BB and AC at codons 54 and 57, respectively, showed higher frequencies than the wild-type genotype (AA) (14.1% versus 12.9% and 28.1% versus 19.4% respectively) in both groups, and this difference was greater in the septic group than in the non-septic group; however, the differences did not reach statistical significance. The B and C allele frequencies were also higher in the septic group than in the non-septic group, but the differences did not reach statistical significance ( p  = 0.282 and 0.394, respectively). The serum levels of MBL were significantly lower in the septic group than in the non-septic group ( p  = 0.028). Conclusion  This study found no association between MBL levels or MBL2 exon 1 genotypes or alleles and neonatal sepsis risk. Further studies with larger sample sizes are needed to determine the role of the MBL2 gene as a risk factor and early predictor of neonatal sepsis.

Entities:  

Keywords:  gene polymorphism; mannose-binding lectin; neonatal sepsis

Year:  2018        PMID: 30464858      PMCID: PMC6246104          DOI: 10.1055/s-0038-1675801

Source DB:  PubMed          Journal:  J Pediatr Genet        ISSN: 2146-460X


  32 in total

1.  Mannose-binding lectin serum levels in neonatal sepsis and septic shock.

Authors:  Walid Abdel Wahab Mohamed; Mohamed Abdullatif Saeed
Journal:  J Matern Fetal Neonatal Med       Date:  2011-06-01

2.  Sepsis in acute myeloid leukaemia patients receiving high-dose chemotherapy: no impact of chitotriosidase and mannose-binding lectin polymorphisms.

Authors:  Anja Klostergaard; Rudi Steffensen; Jens K Møller; Niels Peterslund; Caroline Juhl-Christensen; Ingolf Mølle
Journal:  Eur J Haematol       Date:  2010-03-12       Impact factor: 2.997

Review 3.  Mannose-binding lectin: clinical implications for infection, transplantation, and autoimmunity.

Authors:  Lee H Bouwman; Bart O Roep; Anja Roos
Journal:  Hum Immunol       Date:  2006-04-17       Impact factor: 2.850

4.  High prevalence of mannose-binding lectin (MBL) deficiency in premature neonates.

Authors:  F N J Frakking; N Brouwer; D Zweers; M P Merkus; T W Kuijpers; M Offringa; K M Dolman
Journal:  Clin Exp Immunol       Date:  2006-07       Impact factor: 4.330

5.  A simple salting out procedure for extracting DNA from human nucleated cells.

Authors:  S A Miller; D D Dykes; H F Polesky
Journal:  Nucleic Acids Res       Date:  1988-02-11       Impact factor: 16.971

6.  Disease-associated mutations in human mannose-binding lectin compromise oligomerization and activity of the final protein.

Authors:  Flemming Larsen; Hans O Madsen; Robert B Sim; Claus Koch; Peter Garred
Journal:  J Biol Chem       Date:  2004-02-05       Impact factor: 5.157

7.  Low-mannose-binding lectin levels in susceptibility to neonatal sepsis in preterm neonates with fetal inflammatory response syndrome.

Authors:  Ozgur Ozdemir; Ener Cagri Dinleyici; Neslihan Tekin; Omer Colak; M Arif Aksit
Journal:  J Matern Fetal Neonatal Med       Date:  2010-09

Review 8.  Mannose-binding lectin genetics: from A to Z.

Authors:  Peter Garred
Journal:  Biochem Soc Trans       Date:  2008-12       Impact factor: 5.407

9.  Mannose-binding lectin polymorphisms and the risk of sepsis: evidence from a meta-analysis.

Authors:  A-Q Zhang; C-L Yue; W Pan; J-W Gao; L Zeng; W Gu; J-X Jiang
Journal:  Epidemiol Infect       Date:  2014-01-07       Impact factor: 4.434

Review 10.  Neonatal sepsis: an old problem with new insights.

Authors:  Birju A Shah; James F Padbury
Journal:  Virulence       Date:  2013-11-01       Impact factor: 5.882
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  3 in total

Review 1.  Association between innate immunity gene polymorphisms and neonatal sepsis development: a systematic review and meta-analysis.

Authors:  Tamara Sljivancanin Jakovljevic; Jelena Martic; Jelena Jacimovic; Nadja Nikolic; Jelena Milasin; Tanja Lazić Mitrović
Journal:  World J Pediatr       Date:  2022-06-06       Impact factor: 9.186

2.  Role of MBL2 Polymorphisms in Sepsis and Survival: A Pilot Study and In Silico Analysis.

Authors:  Mohammed Y Behairy; Ali A Abdelrahman; Hoda Y Abdallah; Emad El-Deen A Ibrahim; Hany R Hashem; Anwar A Sayed; Marwa M Azab
Journal:  Diagnostics (Basel)       Date:  2022-02-11

3.  Mannose-binding lectin serum levels and (Gly54asp) gene polymorphism in recurrent aphthous stomatitis: A case-control study.

Authors:  Shereen A Baioumy; Shaimaa H Fouad; Shaimaa A Abdalgeleel; Ahmed A Baiomy; Dina E Sallam; Sara I Taha
Journal:  Int J Immunopathol Pharmacol       Date:  2021 Jan-Dec       Impact factor: 3.219
  3 in total

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