An open protocol for modeling T Cell Clonotype repertoires using TCRβ CDR3 sequences

Author:

Gurun Burcu1ORCID,Horton Wesley2,Murugan Dhaarini2ORCID,Zhu Biqing3ORCID,Leyshock Patrick2,Kumar Sushil2,Byrne Katelyn T.2ORCID,Vonderheide Robert H.4,Margolin Adam A.5,Mori Motomi6ORCID,Spellman Paul T.2ORCID,Coussens Lisa M.2,Speed Terence P.7ORCID

Affiliation:

1. Oregon Health and Science University

2. Oregon Health & Science University Hospital

3. Yale University

4. Upenn: University of Pennsylvania

5. Khosla Ventures

6. St Jude Children's Research Hospital

7. WEHI: Walter and Eliza Hall Institute of Medical Research

Abstract

Abstract T cell receptor repertoires can be profiled using next generation sequencing (NGS) to measure and monitor adaptive dynamical changes in response to disease and other perturbations. Genomic DNA-based bulk sequencing is cost-effective but necessitates multiplex target amplification using multiple primer pairs with highly variable amplification efficiencies. Here, we utilize an equimolar primer mixture and propose a single statistical normalization step that efficiently corrects for amplification bias post sequencing. Using samples analyzed by both our open protocol and a commercial solution, we show high concordance between bulk clonality metrics. This approach is an inexpensive and open-source alternative to commercial solutions.

Publisher

Research Square Platform LLC

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