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The production of antibodies (Abs) with high affinity and pathogen neutralization potential is crucial for preventing and fighting pathogen infection. To produce such Abs, naïve B cells are activated in response to cognate antigen and subsequently undergo rounds of somatic hypermutation and selection in germinal centers, specialized microanatomical sites in secondary lymphoid organs. This process of affinity maturation is tightly regulated by a specialized subset of CD4 T cells named T follicular helper (Tfh) cells. Our laboratory is interested in dissecting the complex biology of Tfh cells. Understanding (1) how Tfh differentiation is regulated and (2) by what means Tfh cells enable effective B cell responses are two major research goals that our group seeks to address by using a multidisciplinary approach that combines cellular and molecular immunology as well as transcriptomics:
1) Tfh cells undergo a multistage process to become fully differentiated effector cells. This sophisticated process is driven by a network of cytokines and costimulatory molecules that has been only partially elucidated. To uncover novel regulators of human Tfh differentiation, we set up a high throughput in vitro screen of a custom library of human secreted or cell surface proteins. The screen identified the cytokine activin A as a strong hit in promoting the differentiation of Tfh-like cells from human naïve CD4 T cells activated in vitro (Locci et al. Nat. Immunol., 2016). We found that activin A orchestrates the expression of multiple Tfh-associated genes, including PD-1, CXCR5 and CXCL13, in a highly specific fashion. Ongoing and future studies are aimed at dissecting the molecular mechanism by which activin A regulates human Tfh differentiation as well as the role played by activin A in Tfh cell differentiation and B cell helper function in vivo. Furthermore, additional candidates are currently being evaluated for their capacity to mold Tfh cell differentiation.
2) In germinal centers, bona fide Tfh cells regulate the survival and selection of high affinity B cells by delivering ‘help’ signals via cytokines and membrane-bound costimulatory receptors. Thus far, the functional mediators utilized by Tfh cells to provide help to germinal center B cells are poorly understood. Studies on human memory Tfh cells from peripheral blood, which are considered as the circulating counterpart of lymphoid tissue bona fide Tfh cells, revealed a high degree of functional heterogeneity in the Tfh cell population. We described the blood Th1-depleted PD-1+CXCR3- cells as the memory Tfh cell subset with the highest B cell helper capacity (Locci et al. Immunity 2013). Our group seeks to untangle the functional heterogeneity of human memory and bona fide Tfh and unmask crucial mediators of B cell help by performing single-cell transcriptional profiling coupled to functional studies.
The production of antibodies (Abs) with high affinity and pathogen neutralization potential is crucial for preventing and fighting pathogen infection. To produce such Abs, naïve B cells are activated in response to cognate antigen and subsequently undergo rounds of somatic hypermutation and selection in germinal centers, specialized microanatomical sites in secondary lymphoid organs. This process of affinity maturation is tightly regulated by a specialized subset of CD4 T cells named T follicular helper (Tfh) cells. Our laboratory is interested in dissecting the complex biology of Tfh cells. Understanding (1) how Tfh differentiation is regulated and (2) by what means Tfh cells enable effective B cell responses are two major research goals that our group seeks to address by using a multidisciplinary approach that combines cellular and molecular immunology as well as transcriptomics:
1) Tfh cells undergo a multistage process to become fully differentiated effector cells. This sophisticated process is driven by a network of cytokines and costimulatory molecules that has been only partially elucidated. To uncover novel regulators of human Tfh differentiation, we set up a high throughput in vitro screen of a custom library of human secreted or cell surface proteins. The screen identified the cytokine activin A as a strong hit in promoting the differentiation of Tfh-like cells from human naïve CD4 T cells activated in vitro (Locci et al. Nat. Immunol., 2016). We found that activin A orchestrates the expression of multiple Tfh-associated genes, including PD-1, CXCR5 and CXCL13, in a highly specific fashion. Ongoing and future studies are aimed at dissecting the molecular mechanism by which activin A regulates human Tfh differentiation as well as the role played by activin A in Tfh cell differentiation and B cell helper function in vivo. Furthermore, additional candidates are currently being evaluated for their capacity to mold Tfh cell differentiation.
2) In germinal centers, bona fide Tfh cells regulate the survival and selection of high affinity B cells by delivering ‘help’ signals via cytokines and membrane-bound costimulatory receptors. Thus far, the functional mediators utilized by Tfh cells to provide help to germinal center B cells are poorly understood. Studies on human memory Tfh cells from peripheral blood, which are considered as the circulating counterpart of lymphoid tissue bona fide Tfh cells, revealed a high degree of functional heterogeneity in the Tfh cell population. We described the blood Th1-depleted PD-1+CXCR3- cells as the memory Tfh cell subset with the highest B cell helper capacity (Locci et al. Immunity 2013). Our group seeks to untangle the functional heterogeneity of human memory and bona fide Tfh and unmask crucial mediators of B cell help by performing single-cell transcriptional profiling coupled to functional studies.
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Papers共 63 篇Author StatisticsCo-AuthorSimilar Experts
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CLINICAL AND TRANSLATIONAL MEDICINEno. 3 (2024): e1608-e1608
Kai Markus Schneider,Niklas Blank,Yelina Alvarez, Katharina Thum,Patrick Lundgren,Lev Litichevskiy, Madeleine Sleeman,Klaas Bahnsen,Jihee Kim, Simon Kardo,Shaan Patel,Lenka Dohnalova,Giulia T. Uhr,Helene C. Descamps, Susanna Kircher,Alana M. McSween,Ashkan Rezazadeh Ardabili,Kelsey M. Nemec,Monica T. Jimenez,Lila G. Glotfelty, Joshua D. Eisenberg,Emma E. Furth,Jorge Henao-Mejia,F. Chris Bennett,Marie J. Pierik,Marielle Romberg-Camps,Zlatan Mujagic,Marco Prinz,Carolin V. Schneider,E. John Wherry,Meenakshi Bewtra,Robert O. Heuckeroth,Maayan Levy,Christoph A. Thaiss
Cellno. 13 (2023): 2823-2838.e20
William F. F. Kindschuh,Federico Baldini,Martin C. C. Liu,Jingqiu Liao, Yoli Meydan,Harry H. H. Lee, Almut Heinken, Ines Thiele, Christoph A. A. Thaiss,Maayan Levy,Tal Korem
Andrea C. Wong, Ashwarya Devason, Iboro C. Umana,Timothy Cox,Lenka Dohnalova,Nuala J. Meyer,Benjamin Abramoff,Sara Cherry,Christoph Thaiss,Maayan Levy
Journal of Immunologyno. 1 (2023): 236.21-236.21
Patrick Lundgren,Prateek V. Sharma,Lenka Dohnalová,Kyle Coleman,Giulia T. Uhr, Susanna Kircher,Lev Litichevskiy,Klaas Bahnsen,Hélène C. Descamps,Christina Demetriadou, Jacqueline Chan,Karthikeyani Chellappa,Timothy O. Cox, Yael Heyman,Sarshan R. Pather,Clarissa Shoffler,Christopher Petucci,Ophir Shalem,Arjun Raj,Joseph A. Baur,Nathaniel W. Snyder,Kathryn E. Wellen,Maayan Levy,Patrick Seale,Mingyao Li,Christoph A. Thaiss
Nature Metabolismno. 10 (2023): 1691-1705
Jihee Kim,Kirti Nath,Kurt Schmidlin,Helen Schaufelberger, Christiana Quattropani, Simone Vannini, Sandro Mossi,Miriam Thumshirn,Michael Manz,Lev Litichevskiy,Jiaxin Fan,Oxana Dmitrieva-Posocco,Mingyao Li,Maayan Levy,Primo Schär,Marcel Zwahlen,Christoph A. Thaiss,Kaspar Truninger
FRONTIERS IN CELLULAR AND INFECTION MICROBIOLOGY (2023)
Andrea C. Wong, Ashwarya S. Devason, Iboro C. Umana,Timothy O. Cox,Lenka Dohnalova,Lev Litichevskiy, Jonathan Perla,Patrick Lundgren,Zienab Etwebi,Luke T. Izzo,Jihee Kim, Monika Tetlak,Helene C. Descamps,Simone L. Park, Stephen Wisser,Aaron D. McKnight,Ryan D. Pardy,Junwon Kim,Niklas Blank,Shaan Patel, Katharina Thum, Sydney Mason,Jean-Christophe Beltra,Michael F. Michieletto,Shin Foong Ngiow,Brittany M. Miller,Megan J. Liou,Bhoomi Madhu,Oxana Dmitrieva-Posocco, Alex S. Huber,Peter Hewins,Christopher Petucci, Candice P. Chu,Gwen Baraniecki-Zwil,Leila B. Giron,Amy E. Baxter,Allison R. Greenplate, Charlotte Kearns,Kathleen Montone,Leslie A. Litzky,Michael Feldman,Jorge Henao-Mejia, Boris Striepen,Holly Ramage,Kellie A. Jurado,Kathryn E. Wellen,Una O'Doherty,Mohamed Abdel-Mohsen,Alan L. Landay,Ali Keshavarzian,Timothy J. Henrich,Steven G. Deeks,Michael J. Peluso,Nuala J. Meyer,E. John Wherry,Benjamin A. Abramoff,Sara Cherry,Christoph A. Thaiss,Maayan Levy
Cellno. 22 (2023): 4851-4867.e20
Lenka Dohnalova,Patrick Lundgren,Jamie R. E. Carty,Nitsan Goldstein,Sebastian L. Wenski,Pakjira Nanudorn,Sirinthra Thiengmag,Kuei-Pin Huang,Lev Litichevskiy,Helene C. Descamps,Karthikeyani Chellappa, Ana Glassman,Susanne Kessler,Jihee Kim,Timothy O. Cox,Oxana Dmitrieva-Posocco,Andrea C. Wong,Erik L. Allman,Soumita Ghosh,Nitika Sharma,Kasturi Sengupta,Belinda Cornes, Nitai Dean,Gary A. Churchill,Tejvir S. Khurana,Mark A. Sellmyer,Garret A. FitzGerald,Andrew D. Patterson,Joseph A. Baur,Amber L. Alhadeff,Eric J. N. Helfrich,Maayan Levy,J. Nicholas Betley,Christoph A. Thaiss
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#Papers: 64
#Citation: 10387
H-Index: 32
G-Index: 64
Sociability: 6
Diversity: 0
Activity: 1
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