论文信息 - Computational Model Reveals Limited Correlation between Germinal Center B-Cell Subclone Abundancy and Affinity: Implications for Repertoire Sequencing - 字舞流文

Computational Model Reveals Limited Correlation between Germinal Center B-Cell Subclone Abundancy and Affinity: Implications for Repertoire Sequencing

Immunoglobulin repertoire sequencing has successfully been applied to identify expanded antigen-activated B-cell clones that play a role in the pathogenesis of immune disorders. One challenge is the selection of the Ag-specific B cells from the measured repertoire for downstream analyses. A general feature of an immune response is the expansion of specific clones resulting in a set of subclones with common ancestry varying in abundance and in the number of acquired somatic mutations. The expanded subclones are expected to have BCR affinities for the Ag higher than the affinities of the naive B cells in the background population. For these reasons, several groups successfully proceeded or suggested selecting highly abundant subclones from the repertoire to obtain the Ag-specific B cells. Given the nature of affinity maturation one would expect that abundant subclones are of high affinity but since repertoire sequencing only provides information about abundancies, this can only be verified with additional experiments, which are very labor intensive. Moreover, this would also require knowledge of the Ag, which is often not available for clinical samples. Consequently, in general we do not know if the selected highly abundant subclone(s) are also the high(est) affinity subclones. Such knowledge would likely improve the selection of relevant subclones for further characterization and Ag screening. Therefore, to gain insight in the relation between subclone abundancy and affinity, we developed a computational model that simulates affinity maturation in a single GC while tracking individual subclones in terms of abundancy and affinity. We show that the model correctly captures the overall GC dynamics, and that the amount of expansion is qualitatively comparable to expansion observed from B cells isolated from human lymph nodes. Analysis of the fraction of high- and low-affinity subclones among the unexpanded and expanded subclones reveals a limited correlation between abundancy and affinity and shows that the low abundant subclones are of highest affinity. Thus, our model suggests that selecting highly abundant subclones from repertoire sequencing experiments would not always lead to the high(est) affinity B cells. Consequently, additional or alternative selection approaches need to be applied.

Polina Reshetova | P. Tak | A. V. van Kampen | N. de Vries | M. Doorenspleet | B. V. van Schaik | R. Esveldt | J. Guikema | Niek de Vries | Antoine H. C. van Kampen | Marieke E. Doorenspleet | Paul-Peter Tak | Barbera D. C. van Schaik | Paul L. Klarenbeek | Rebecca E. E. Esveldt | Jeroen E. J. Guikema | P. Klarenbeek | P. Reshetova | Polina Reshetova

[1] M. Shlomchik,et al. A Temporal Switch in the Germinal Center Determines Differential Output of Memory B and Plasma Cells. , 2014, Immunity.

[2] D. Runia,et al. Title of the Work , 2019, Philo of Alexandria: On the Life of Abraham.

[3] W. Robinson. Sequencing the functional antibody repertoire—diagnostic and therapeutic discovery , 2015, Nature Reviews Rheumatology.

[4] Mathieu Rouard,et al. IMGT unique numbering for immunoglobulin and T cell receptor constant domains and Ig superfamily C-like domains. , 2005, Developmental and comparative immunology.

[5] Frank Baas,et al. Human T-cell memory consists mainly of unexpanded clones. , 2010, Immunology letters.

[6] P. Tak,et al. Hunting for the pathogenesis of rheumatoid arthritis: core-needle biopsy of inguinal lymph nodes as a new research tool , 2012, Annals of the rheumatic diseases.

[7] R Core Team,et al. R: A language and environment for statistical computing. , 2014 .

[8] F. Baas,et al. Rheumatoid arthritis synovial tissue harbours dominant B-cell and plasma-cell clones associated with autoreactivity , 2013, Annals of the rheumatic diseases.

[9] C. Berek,et al. Maturation of the immune response in germinal centers , 1991, Cell.

[10] R C Stevens,et al. Structural insights into the evolution of an antibody combining site. , 1997, Science.

[11] Steven H. Kleinstein,et al. The mutation patterns in B-cell immunoglobulin receptors reflect the influence of selection acting at multiple time-scales , 2015, Philosophical Transactions of the Royal Society B: Biological Sciences.

[12] Armin A. Weiser,et al. Is There a Typical Germinal Center? A Large-Scale Immunohistological Study on the Cellular Composition of Germinal Centers during the Hapten-Carrier–Driven Primary Immune Response in Mice , 2011, The Journal of Immunology.

[13] S H Kleinstein,et al. Toward quantitative simulation of germinal center dynamics: biological and modeling insights from experimental validation. , 2001, Journal of theoretical biology.

[14] Karline Soetaert,et al. Solving Differential Equations in R: Package deSolve , 2010 .

[15] Eline T. Luning Prak,et al. The analysis of clonal expansions in normal and autoimmune B cell repertoires , 2015, Philosophical Transactions of the Royal Society B: Biological Sciences.

[16] K. Pang,et al. Increasing Viral Dose Causes a Reversal in CD8+ T Cell Immunodominance during Primary Influenza Infection due to Differences in Antigen Presentation, T Cell Avidity, and Precursor Numbers , 2013, The Journal of Immunology.

[17] D. Calado,et al. Germinal Centers , 2017, Methods in Molecular Biology.

[18] Uri Hershberg,et al. Persistence and selection of an expanded B-cell clone in the setting of rituximab therapy for Sjögren’s syndrome , 2014, Arthritis Research & Therapy.

[19] U. Klein,et al. Dynamics of B cells in germinal centres , 2015, Nature Reviews Immunology.

[20] David Nemazee,et al. Tailored Immunogens Direct Affinity Maturation toward HIV Neutralizing Antibodies , 2016, Cell.

[21] G. B. Karlsson Hedestam,et al. Production of individualized V gene databases reveals high levels of immunoglobulin genetic diversity , 2016, Nature Communications.

[22] Michael Meyer-Hermann,et al. Germinal Center Dynamics Revealed by Multiphoton Microscopy with a Photoactivatable Fluorescent Reporter , 2010, Cell.

[23] F. Baas,et al. Inflamed target tissue provides a specific niche for highly expanded T-cell clones in early human autoimmune disease. , 2012, Annals of the rheumatic diseases.

[24] Peter N. Robinson,et al. IMSEQ - a fast and error aware approach to immunogenetic sequence analysis , 2015, Bioinform..

[25] Marie-Paule Lefranc,et al. Immunoglobulin and T Cell Receptor Genes: IMGT® and the Birth and Rise of Immunoinformatics , 2014, Front. Immunol..

[26] Tilo Beyer,et al. A possible role of chemotaxis in germinal center formation. , 2002, International immunology.

[27] J. Calis,et al. Characterizing immune repertoires by high throughput sequencing: strategies and applications. , 2014, Trends in immunology.

[28] W. Robinson,et al. High-throughput sequencing of natively paired antibody chains provides evidence for original antigenic sin shaping the antibody response to influenza vaccination. , 2014, Clinical immunology.

[29] M. Gorfine,et al. Antigen-driven selection in germinal centers as reflected by the shape characteristics of immunoglobulin gene lineage trees: a large-scale simulation study. , 2008, Journal of theoretical biology.

[30] Karline Soetaert,et al. Inverse Modelling, Sensitivity and Monte Carlo Analysis in R Using Package FME , 2010 .

[31] M. Shlomchik,et al. Clone: a Monte-Carlo computer simulation of B cell clonal expansion, somatic mutation, and antigen-driven selection. , 1998, Current topics in microbiology and immunology.

[32] D. Tarlinton,et al. Determining germinal centre B cell fate. , 2012, Trends in immunology.

[33] Scott D Boyd,et al. Convergent antibody signatures in human dengue. , 2013, Cell host & microbe.

[34] Michael Meyer-Hermann,et al. A mathematical model for the germinal center morphology and affinity maturation. , 2002, Journal of theoretical biology.

[35] D. E. Kelley,et al. Transcriptional and posttranscriptional control of immunoglobulin mRNA production during B lymphocyte development , 1986, Nucleic Acids Res..

[36] J. Singh,et al. Why are there so few key mutant clones? The influence of stochastic selection and blocking on affinity maturation in the germinal center. , 2003, International immunology.

[37] G. Yaari,et al. Practical guidelines for B-cell receptor repertoire sequencing analysis , 2015, Genome Medicine.

[38] J. Galson,et al. Identification of Antigen-Specific B-Cell Receptor Sequences from the Total B-Cell Repertoire. , 2015, Critical reviews in immunology.

[39] Steven H. Kleinstein,et al. B cells populating the multiple sclerosis brain mature in the draining cervical lymph nodes , 2014, Science Translational Medicine.

[40] Uri Hershberg,et al. Improved methods for detecting selection by mutation analysis of Ig V region sequences. , 2008, International immunology.

[41] Michael Meyer-Hermann,et al. Visualizing antibody affinity maturation in germinal centers , 2016, Science.

[42] Anna Tramontano,et al. Igs Expressed by Chronic Lymphocytic Leukemia B Cells Show Limited Binding-Site Structure Variability , 2013, The Journal of Immunology.

[43] Marie-Paule Lefranc,et al. IMGT , the international ImMunoGeneTics information system , 2003 .

[44] G. Kelsoe,et al. In situ studies of the primary immune response to (4-hydroxy-3- nitrophenyl)acetyl. III. The kinetics of V region mutation and selection in germinal center B cells , 1993, The Journal of experimental medicine.

[45] Alla Lapidus,et al. IgRepertoireConstructor: a novel algorithm for antibody repertoire construction and immunoproteogenomics analysis , 2015, Bioinform..

[46] Michel C. Nussenzweig,et al. Clonal selection in the germinal centre by regulated proliferation and hypermutation , 2014, Nature.

[47] A S Perelson,et al. Somatic mutation leads to efficient affinity maturation when centrocytes recycle back to centroblasts. , 1997, Journal of immunology.

[48] G. Kelsoe,et al. In situ studies of the primary immune response to (4-hydroxy-3- nitrophenyl)acetyl. I. The architecture and dynamics of responding cell populations , 1991, The Journal of experimental medicine.

[49] M. Shlomchik,et al. Germinal center selection and the development of memory B and plasma cells , 2012, Immunological reviews.

[50] Paul Leonard,et al. Measuring antibody-antigen binding kinetics using surface plasmon resonance. , 2012, Methods in molecular biology.

[51] Yan Wang,et al. The mouse antibody heavy chain repertoire is germline-focused and highly variable between inbred strains , 2015, Philosophical Transactions of the Royal Society B: Biological Sciences.

[52] K. Rajewsky,et al. Tracing B cell development in human germinal centres by molecular analysis of single cells picked from histological sections. , 1993, The EMBO journal.

[53] Armin A. Weiser,et al. Recirculation of germinal center B cells: a multilevel selection strategy for antibody maturation , 2007, Immunological reviews.

[54] V. Giudicelli,et al. IMGT unique numbering for immunoglobulin and T cell receptor variable domains and Ig superfamily V-like domains. , 2003, Developmental and comparative immunology.

[55] R. Hohlfeld,et al. Novel approaches for identifying target antigens of autoreactive human B and T cells , 2009, Seminars in Immunopathology.

[56] J. Macartney,et al. Cell kinetics of the germinal center reaction ‐ a stathmokinetic study , 1992, European journal of immunology.

[57] Evgeny S. Egorov,et al. High-quality full-length immunoglobulin profiling with unique molecular barcoding , 2016, Nature Protocols.

[58] Paul D. W. Kirk,et al. MEANS: python package for Moment Expansion Approximation, iNference and Simulation , 2016, Bioinform..

[59] Armin A. Weiser,et al. Broad Volume Distributions Indicate Nonsynchronized Growth and Suggest Sudden Collapses of Germinal Center B Cell Populations , 2010, The Journal of Immunology.

[60] P. Gearhart,et al. Early onset of somatic mutation in immunoglobulin VH genes during the primary immune response , 1989, The Journal of experimental medicine.

[61] F. Baas,et al. Immunoglobulin G4+ clones identified by next‐generation sequencing dominate the B cell receptor repertoire in immunoglobulin G4 associated cholangitis , 2013, Hepatology.

[62] Ron Unger,et al. IgTree: creating Immunoglobulin variable region gene lineage trees. , 2008, Journal of immunological methods.

[63] W. J. Kent,et al. BLAT--the BLAST-like alignment tool. , 2002, Genome research.

[64] Michael Meyer-Hermann,et al. Germinal center B cells govern their own fate via antibody feedback , 2013, The Journal of experimental medicine.

[65] Xun Xu,et al. IMonitor: A Robust Pipeline for TCR and BCR Repertoire Analysis , 2015, Genetics.

[66] Garnett Kelsoe,et al. Predicted and inferred waiting times for key mutations in the germinal centre reaction: Evidence for stochasticity in selection , 1998, Immunology and cell biology.

[67] Jun Zhang,et al. Sites of specific B cell activation in primary and secondary responses to T cell‐dependent and T cell‐independent antigens , 1991, European journal of immunology.

[68] R Mehr,et al. Reconciling repertoire shift with affinity maturation: the role of deleterious mutations. , 1999, Journal of immunology.