Improved methods for detecting selection by mutation analysis of Ig V region sequences

doi:10.1093/intimm/dxn026

International Immunology Advance Access originally published online on April 7, 2008
International Immunology 2008 20(5):683-694; doi:10.1093/intimm/dxn026

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Improved methods for detecting selection by mutation analysis of Ig V region sequences

Uri Hershberg¹^,2, Mohamed Uduman³, Mark J. Shlomchik¹^,2 and Steven H. Kleinstein³^,4

¹ Department of Laboratory Medicine
² Department of Immunobiology
³ Interdepartmental Program in Computational Biology and Bioinformatics
⁴ Department of Pathology, Yale University School of Medicine, Yale University, The Anlyan Center, New Haven, CT 06520, USA

Correspondence to: S.H. Kleinstein; E-mail: steven.kleinstein{at}yale.edu

Statistical methods based on the relative frequency of replacementmutations in B lymphocyte Ig V region sequences have been widelyused to detect the forces of selection that shape the B cellrepertoire. However, current methods produce an unexpectedlyhigh frequency of false positives and are sensitive to intrinsicbiases of somatic hypermutation that can give the appearanceof selection. The new statistical test proposed here providesa better trade-off between sensitivity and specificity comparedwith previous approaches. The low specificity of existing methodswas shown in silico to result from an interaction between theeffects of positive and negative selection. False detectionof positive selection was confirmed in vivo through a re-analysisof published sequence data from diffuse large B cell lymphomas,highlighting the need for re-analysis of some existing studies.The sensitivity of the proposed method to detect selection wasvalidated using new Ig transgenic mouse models in which positiveselection was expected to be a significant force, as well aswith a simulation-based approach. Previous concerns that intrinsicbiases of somatic hypermutation could give the appearance ofselection were addressed by extending the current mutation modelsto more fully account for the impact of microsequence on relativemutability and to include transition bias. High specificitywas confirmed using a large set of non-productively rearrangedIg sequences. These results show that selection can be detectedin vivo with high specificity using the new method proposedhere, allowing greater insight into the existence and directionof antigen-driven selection.

Keywords: adaptive immunity, affinity maturation, B cells, cancer, germinal center

Transmitting editor: D. Tarlinton

Received 2 November 2007, accepted 14 February 2008.

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