| Literature DB >> 30626755 |
Pablo Vieyra-Garcia1,2, Jack D Crouch1, John T O'Malley1, Edward W Seger1, Chao H Yang1, Jessica E Teague1, Anna Maria Vromans1, Ahmed Gehad1, Thet Su Win1, Zizi Yu3, Elizabeth L Lowry1, Jung-Im Na1,4, Alain H Rook5, Peter Wolf2, Rachael A Clark1.
Abstract
Psoralen plus UVA (PUVA) is an effective therapy for mycosis fungoides (MF), the skin-limited variant of cutaneous T cell lymphoma (CTCL). In low-burden patients, PUVA reduced or eradicated malignant T cells and induced clonal expansion of CD8+ T cells associated with malignant T cell depletion. High-burden patients appeared to clinically improve but large numbers of malignant T cells persisted in skin. Clinical improvement was linked to turnover of benign T cell clones but not to malignant T cell reduction. Benign T cells were associated with the Th2-recruiting chemokine CCL18 before therapy and with the Th1-recruiting chemokines CXCL9, CXCL10, and CXCL11 after therapy, suggesting a switch from Th2 to Th1. Inflammation was correlated with OX40L and CD40L gene expression; immunostaining localized these receptors to CCL18-expressing c-Kit+ dendritic cells that clustered together with CD40+OX40+ benign and CD40+CD40L+ malignant T cells, creating a proinflammatory synapse in skin. Our data suggest that visible inflammation in CTCL results from the recruitment and activation of benign T cells by c-Kit+OX40L+CD40L+ dendritic cells and that this activation may provide tumorigenic signals. Targeting c-Kit, OX40, and CD40 signaling may be novel therapeutic avenues for the treatment of MF.Entities:
Keywords: Dermatology; Immunology; Lymphomas
Year: 2019 PMID: 30626755 PMCID: PMC6485670 DOI: 10.1172/jci.insight.124233
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708