ID

45688

Description

Principal Investigator: Ning Jiang, PhD, University of Texas at Austin, Austin, TX, USA MeSH: Malaria,Malaria, Falciparum https://www.ncbi.nlm.nih.gov/projects/gap/cgi-bin/study.cgi?study_id=phs001209 This study describes a novel Immune Repertoire Sequencing technique, termed Molecular Identifier Clustering-based Immune Repertoire Sequencing (MIDCIRS), to reduce sequencing error while maintaining extremely high coverage and applies this technique to investigate the differential immune response to malaria between infants and toddlers. Despite a lower somatic hypermutation load, we found an unexpectedly high level of competency within the infant antibody repertoire, particularly the ability to diversify B cell clonal lineages upon acute infection. Detailed clonal lineage analysis encompassing lineages containing sequences from both pre- and acute malaria timepoints revealed an increase in somatic hypermutations upon acute infection. Further analysis on pre-malaria memory B cell containing lineages in toddlers who had previously been exposed to malaria provides evidence for the capacity of memory B cells to continue to mutate and isotype switch.

Lien

dbGaP study = phs001209

Mots-clés

  1. 03/05/2023 03/05/2023 - Simon Heim
Détendeur de droits

Ning Jiang, PhD, University of Texas at Austin, Austin, TX, USA

Téléchargé le

3 mai 2023

DOI

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Licence

Creative Commons BY 4.0

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dbGaP phs001209 MIDCIRS Reveals Antibody Diversification in Young Children with Malaria

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