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Alternative splice variants and germline polymorphisms in human immunoglobulin light chain genes

View ORCID ProfileIvana Mikocziova, Ayelet Peres, Moriah Gidoni, View ORCID ProfileVictor Greiff, View ORCID ProfileGur Yaari, View ORCID ProfileLudvig M. Sollid
doi: https://doi.org/10.1101/2021.02.05.429934
Ivana Mikocziova
1K.G.Jebsen Centre for Coeliac Disease Research, Institute of Clinical Medicine, University of Oslo, 0372 Oslo, Norway
3Department of Immunology, Oslo University Hospital, 0372 Oslo, Norway
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  • ORCID record for Ivana Mikocziova
Ayelet Peres
2Faculty of Engineering, Bar Ilan University, Ramat Gan 5290002, Israel
4Bar Ilan Institute of Nanotechnologies and Advanced Materials, Bar Ilan University, Ramat Gan 5290002, Israel
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Moriah Gidoni
2Faculty of Engineering, Bar Ilan University, Ramat Gan 5290002, Israel
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Victor Greiff
3Department of Immunology, Oslo University Hospital, 0372 Oslo, Norway
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Gur Yaari
2Faculty of Engineering, Bar Ilan University, Ramat Gan 5290002, Israel
4Bar Ilan Institute of Nanotechnologies and Advanced Materials, Bar Ilan University, Ramat Gan 5290002, Israel
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Ludvig M. Sollid
1K.G.Jebsen Centre for Coeliac Disease Research, Institute of Clinical Medicine, University of Oslo, 0372 Oslo, Norway
3Department of Immunology, Oslo University Hospital, 0372 Oslo, Norway
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  • For correspondence: l.m.sollid@medisin.uio.no
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ABSTRACT

Immunoglobulin loci are rich in germline polymorphisms and identification of novel polymorphic variants can be facilitated by germline inference of B cell receptor repertoires. Germline gene inference is complicated by somatic hypermutations, errors arising from PCR amplification, and DNA sequencing as well as from the varying length of reference alleles. Inference of light chain genes is even more challenging than inference of heavy chain genes due to large gene duplication events on the kappa locus as well as absence of D genes in the rearranged light chain transcripts. Here, we analyzed the light chain cDNA sequences from naïve BCR repertoires of a Norwegian cohort of 100 individuals. We optimized light chain allele inference by tweaking parameters within TIgGER functions, extending the germline reference sequences, and establishing mismatch frequency patterns at polymorphic positions to filter out false positive candidates. As a result, we identified 48 previously unreported variants of light chain variable genes. Altogether, we selected 14 candidates for novel light chain polymorphisms for validation and successfully validated 11 by Sanger sequencing. Additional clustering of light chain 5’UTR, L-PART1 and L-PART2 revealed partial intron retention in alternative splice variants in 11 kappa and 9 lambda V alleles. The alternatively spliced transcripts were only observed in genes with low expression levels, suggesting a possible role in expression regulation. Our results provide novel insight into germline variation in human light chain immunoglobulin loci.

Competing Interest Statement

The authors have declared no competing interest.

Footnotes

  • ↵5 Shared First authors.

  • ↵6 Shared Senior authors.

Copyright 
The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. All rights reserved. No reuse allowed without permission.
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Posted February 06, 2021.
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Alternative splice variants and germline polymorphisms in human immunoglobulin light chain genes
Ivana Mikocziova, Ayelet Peres, Moriah Gidoni, Victor Greiff, Gur Yaari, Ludvig M. Sollid
bioRxiv 2021.02.05.429934; doi: https://doi.org/10.1101/2021.02.05.429934
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Alternative splice variants and germline polymorphisms in human immunoglobulin light chain genes
Ivana Mikocziova, Ayelet Peres, Moriah Gidoni, Victor Greiff, Gur Yaari, Ludvig M. Sollid
bioRxiv 2021.02.05.429934; doi: https://doi.org/10.1101/2021.02.05.429934

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