Isolated peripheral blood CD4 cells from allergic individuals express CC chemokine receptor (CCR)3 and CCR4 after expansion in vitro. In addition, human T helper type 2 (Th2) cells polarized in vitro selectively express CCR3 and CCR4 at certain stages of activation/differentiation and respond preferentially to the ligands eotaxin and monocyte-derived chemokine (MDC). However, controversy arises when the in vivo significance of this distinct expression is discussed. To address the functional role of CCR3/eotaxin and CCR4/MDC during the in vivo recruitment of Th2 cells, we have transferred effector Th cells into naive mice to induce allergic airway disease. Tracking of these cells after repeated antigen challenge has established that both CCR3/eotaxin and CCR4/MDC axes contribute to the recruitment of Th2 cells to the lung, demonstrating the in vivo relevance of the expression of these receptors on Th2 cells. We have shown that involvement of the CCR3/eotaxin pathway is confined to early stages of the response in vivo, whereas repeated antigen stimulation results in the predominant use of the CCR4/MDC pathway. We propose that effector Th2 cells respond to both CCR3/eotaxin and CCR4/MDC pathways initially, but that a progressive increase in CCR4-positive cells results in the predominance of the CCR4/MDC axis in the long-term recruitment of Th2 cells in vivo.
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17 January 2000
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January 17 2000
Cc Chemokine Receptor (Ccr)3/Eotaxin Is Followed by Ccr4/Monocyte-Derived Chemokine in Mediating Pulmonary T Helper Lymphocyte Type 2 Recruitment after Serial Antigen Challenge in Vivo
Clare M. Lloyd,
Clare M. Lloyd
aMillennium Pharmaceuticals, Inc., Cambridge, Massachusetts 02139
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Tracy Delaney,
Tracy Delaney
aMillennium Pharmaceuticals, Inc., Cambridge, Massachusetts 02139
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Trang Nguyen,
Trang Nguyen
aMillennium Pharmaceuticals, Inc., Cambridge, Massachusetts 02139
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Jane Tian,
Jane Tian
aMillennium Pharmaceuticals, Inc., Cambridge, Massachusetts 02139
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Carlos Martinez-A,
Carlos Martinez-A
bDepartment of Immunology and Oncology, Centro Nacional de Biotecnologia, Consejo Superior de Investigaciones Cientificas, Universidad Autonoma, Centroblanco, E28049 Madrid, Spain
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Anthony J. Coyle,
Anthony J. Coyle
aMillennium Pharmaceuticals, Inc., Cambridge, Massachusetts 02139
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Jose-Carlos Gutierrez-Ramos
Jose-Carlos Gutierrez-Ramos
aMillennium Pharmaceuticals, Inc., Cambridge, Massachusetts 02139
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Clare M. Lloyd
aMillennium Pharmaceuticals, Inc., Cambridge, Massachusetts 02139
Tracy Delaney
aMillennium Pharmaceuticals, Inc., Cambridge, Massachusetts 02139
Trang Nguyen
aMillennium Pharmaceuticals, Inc., Cambridge, Massachusetts 02139
Jane Tian
aMillennium Pharmaceuticals, Inc., Cambridge, Massachusetts 02139
Carlos Martinez-A
bDepartment of Immunology and Oncology, Centro Nacional de Biotecnologia, Consejo Superior de Investigaciones Cientificas, Universidad Autonoma, Centroblanco, E28049 Madrid, Spain
Anthony J. Coyle
aMillennium Pharmaceuticals, Inc., Cambridge, Massachusetts 02139
Jose-Carlos Gutierrez-Ramos
aMillennium Pharmaceuticals, Inc., Cambridge, Massachusetts 02139
Abbreviations used in this paper: AAD, allergic airway disease; BAL, bronchoalveolar lavage; BHR, bronchial hyperresponsiveness; CCR, CC chemokine receptor; hpf, high-power field(s); MDC, monocyte-derived chemokine; Penh, enhanced pause; TARC, thymus and activation-regulated chemokine.
Received:
June 14 1999
Revision Requested:
August 26 1999
Accepted:
October 21 1999
Online ISSN: 1540-9538
Print ISSN: 0022-1007
© 2000 The Rockefeller University Press
2000
The Rockefeller University Press
J Exp Med (2000) 191 (2): 265–274.
Article history
Received:
June 14 1999
Revision Requested:
August 26 1999
Accepted:
October 21 1999
Citation
Clare M. Lloyd, Tracy Delaney, Trang Nguyen, Jane Tian, Carlos Martinez-A, Anthony J. Coyle, Jose-Carlos Gutierrez-Ramos; Cc Chemokine Receptor (Ccr)3/Eotaxin Is Followed by Ccr4/Monocyte-Derived Chemokine in Mediating Pulmonary T Helper Lymphocyte Type 2 Recruitment after Serial Antigen Challenge in Vivo. J Exp Med 17 January 2000; 191 (2): 265–274. doi: https://doi.org/10.1084/jem.191.2.265
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