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NAD+ augmentation by nicotinamide riboside engages SLIT2/ROBO1 signaling to attenuate Th17 inflammation in psoriasis
Kim Han, Rachael J. Klein, Thomas C. Recupero, Anna Chiara Russo, Rahul Sharma, Anand K. Gupta, Shahin Hassanzadeh, Rebecca D. Huffstutler, Pradeep K. Dagur, Bryan Fisk, Neelam R. Redekar, Michael N. Sack
Kim Han, Rachael J. Klein, Thomas C. Recupero, Anna Chiara Russo, Rahul Sharma, Anand K. Gupta, Shahin Hassanzadeh, Rebecca D. Huffstutler, Pradeep K. Dagur, Bryan Fisk, Neelam R. Redekar, Michael N. Sack
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Clinical Research and Public Health Dermatology Immunology

NAD+ augmentation by nicotinamide riboside engages SLIT2/ROBO1 signaling to attenuate Th17 inflammation in psoriasis

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Abstract

BACKGROUND Enhancing NAD+ levels with nicotinamide riboside (NR) confers antiinflammatory effects in human disease, although immunoregulatory mechanisms remain poorly characterized. We previously showed that ex vivo NR supplementation of primary CD4+ T cells from psoriatic individuals dampened immune responsiveness.METHODS To validate this in vivo, we performed a randomized, placebo-controlled NR supplementation study in individuals with mild-to-moderate psoriasis. Participants received oral NR (500 mg twice daily) or matching placebo for 4 weeks, with blood samples collected at baseline and after supplementation. NR reduced Th17 immune responsiveness.RESULTS Bulk CD4+ T cell RNA-seq identified induction of the SLIT-ROBO signaling pathway. NR supplementation increased circulating SLIT2 levels and enhanced SLIT2 production in dermal fibroblasts. Pharmacologic and genetic interrogation in CD4+ T cells and fibroblasts demonstrated that SLIT2, acting through the ROBO1 receptor, inhibited Rho GTPase signaling, thereby attenuating canonical Th17 polarization and fibroblast inflammatory activation.CONCLUSION These findings indicate that NAD+ augmentation exerts anti-inflammatory effects in psoriasis through SLIT2-ROBO1-mediated crosstalk between dermal fibroblasts and circulating CD4+ T cells, leading to suppression of Th17-driven inflammation.TRIAL REGISTRATION ClinicalTrials.gov NCT04271735 (registration date – 2020-08026), NCT01143454 (registration date - 2010-07-21), NCT01778569 (registration date – 2013-01-22), and NCT00001846 (registration date – 2001-01-11).FUNDING The NHLBI Division of Intramural Research (HL005102 – MNS).

Authors

Kim Han, Rachael J. Klein, Thomas C. Recupero, Anna Chiara Russo, Rahul Sharma, Anand K. Gupta, Shahin Hassanzadeh, Rebecca D. Huffstutler, Pradeep K. Dagur, Bryan Fisk, Neelam R. Redekar, Michael N. Sack

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Figure 7

NR reduces fibroblast inflammatory responses via SLIT2 signaling.

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NR reduces fibroblast inflammatory responses via SLIT2 signaling.
(A) SL...
(A) SLIT2 production in skin fibroblasts from participants who were healthy and had psoriasis (n = 4 per group) after NR supplementation. Biopsies collected by punch under local anesthesia (ClinicalTrials.gov Identifiers: NCT01778569 and NCT01143454). Lesional skin used for participants with psoriasis. (B–D) CCL2, CXCL8, and IL-6 secretion measured by 13-plex bead-based multiplex assay. (B) Healthy fibroblasts incubated with Th17 differentiation media (n = 8 replicates, 4 independent experiments). (C) Fibroblasts from healthy (HV) and psoriasis (PS) participants. (D) SLIT2 effects on fibroblasts transfected with control or ROBO1 siRNA (n = 5). (E) Proposed model of NR-mediated immunoregulation. NR increases NAD+ levels and enhances SLIT2 secretion from fibroblasts and other cell types, leading to ROBO1-dependent suppression of the Th17 response. Data: mean ± SEM; statistical analyses: unpaired 2-tailed t test (HV versus PS), paired t test (Veh versus NR), or 1-way ANOVA for multiple-group comparisons. P < 0.05, *P < 0.01, **P < 0.001, ***P < 0.0001. Veh, vehicle.

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