IL-32–producing CD8+ memory T cells define immunoregulatory niches in human cutaneous leishmaniasis
Nidhi S. Dey, … , Shalindra Ranasinghe, Paul M. Kaye
Nidhi S. Dey, … , Shalindra Ranasinghe, Paul M. Kaye
Published May 15, 2025
Citation Information: J Clin Invest. 2025;135(10):e182040. https://doi.org/10.1172/JCI182040.
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Research Article Dermatology Immunology Infectious disease

IL-32–producing CD8+ memory T cells define immunoregulatory niches in human cutaneous leishmaniasis

Abstract

Human cutaneous leishmaniasis (CL) is characterized by chronic skin pathology. Experimental and clinical data suggest that immune checkpoints (ICs) play a crucial role in disease outcome, but the cellular and molecular niches that facilitate IC molecule expression during leishmaniasis are ill defined. In Sri Lankan patients with CL, indoleamine 2,3-dioxygenase 1 (IDO1) and programmed death–ligand 1 (PD-L1) were enriched in skin lesions, and reduced PD-L1 expression early after treatment initiation was predictive of a cure rate following antimonial therapy. Here, we used spatial cell interaction mapping to identify IL-32–expressing CD8+ memory T cells and Tregs as key components of the IDO1/PD-L1 niche in Sri Lankan patients with CL and in patients with distinct forms of dermal leishmaniasis in Brazil and India. Furthermore, the abundance of IL-32+ cells and IL-32+CD8+ T cells at treatment initiation was negatively correlated with the rate of cure in Sri Lankan patients. This study provides insights into the spatial mechanisms underpinning IC expression during CL and offers a strategy for identifying additional biomarkers of treatment response.

Authors

Nidhi S. Dey, Shoumit Dey, Naj Brown, Sujai Senarathne, Luiza Campos Reis, Ritika Sengupta, Jose A.L. Lindoso, Sally R. James, Lesley Gilbert, Dave Boucher, Mitali Chatterjee, Hiro Goto, Shalindra Ranasinghe, Paul M. Kaye

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Figure 3

Visium 55 μm neighborhoods of IDO1+ and CD274+ spots.

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Visium 55 μm neighborhoods of IDO1+ and CD274+ spots. (A) IDO1 and CD274...
(A) IDO1 and CD274 normalized gene expression scatter plot for all Visium spots with thresholds (x = 1.1, y = 0.5) defining IDO1, CD274, IDO1/CD274, or other spot classes. (B) P3 spatial plot by spot class in A. Insets identify the lesion core and dermal T cell–rich regions as inferred from Visium and CosMx datasets. (C) Cytokine, chemokine, and receptor abundance by the expression classes described in A. (DK) Spatial feature plots for cytokines, chemokines, and ILs from C in P3’s lesion core and T cell–rich area. (L–N) Additional selected gene spatial features in the same regions. Panels A and C show data from 6 SL CL patients (P1–P6; see also Supplemental Table 1); others represent data from a single patient.