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Generation of diversity by somatic mutation in the Camelus dromedarius T-cell receptor gamma variable domains

Authors :
Giovanna, Vaccarelli
Rachele, Antonacci
Gianluca, Tasco
Fengtang, Yang
Luca, Giordano
Hassan M, El Ashmaoui
Mohamed S, Hassanane
Serafina, Massari
Rita, Casadio
Salvatrice, Ciccarese
Vaccarelli, G
Antonacci, R
Tasco, G
Yang, F
Giordano, L
El Ashmaoui, Hm
Hassanane, M
Massari, Serafina
Casadio, R
Ciccarese, S.
Vaccarelli G
Antonacci R
Tasco G
Yang F
Giordano L
El Ashmaoui HM
Hassanane MS
Massari S
Casadio R
Ciccarese S
Publication Year :
2012

Abstract

In jawed vertebrates the V-(D)-J rearrangement is the main mechanism generating limitless variations of antigen-specific receptors, immunoglobulins (IGs), and T-cell receptors (TCRs) from few genes. Once the initial diversity is established in primary lymphoid organs, further diversification occurs in IGs by somatic hypermutation, a mechanism from which rearranged TCR genes were thought to be excluded. Here, we report the locus organization and expression of the T-cell receptor gamma (TCRG) genes in the Arabian camel (Camelus dromedarius). Expression data provide evidence that dromedary utilizes only two TCRG V-J genomic arrangements and, as expected, CDR3 contributes the major variability in the V domain. The data also suggest that diversity might be generated by mutation in the productively rearranged TCRGV genes. As for IG genes, the mutational target is biased toward G and C bases and (A/G/T)G(C/T)(A/T) motif (or DGYW). The replacement and synonymous substitutions (R/S) ratios in TCRGV regions are higher for CDR than for framework region, thus suggesting selection toward amino acid changes in CDR. Using the counterpart human TCR γδ receptor as a template, structural models computed adopting a comparative procedure show that nonconservative mutations contribute to diversity in CDR2 and at the γδ V domain interface.

Details

Language :
English
Database :
OpenAIRE
Accession number :
edsair.pmid.dedup....db94e2a5a2dab0ee57351cd452c29eed