MSC transplantation ameliorates depression in lupus by suppressing Th1 cell–shaped synaptic stripping
Xiaojuan Han, Dandan Wang, Liang Chen, Hua Song, Xiulan Zheng, Xin Zhang, Shengnan Zhao, Jun Liang, Tianshu Xu, Zhibin Hu, Lingyun Sun
Xiaojuan Han, Dandan Wang, Liang Chen, Hua Song, Xiulan Zheng, Xin Zhang, Shengnan Zhao, Jun Liang, Tianshu Xu, Zhibin Hu, Lingyun Sun
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Research Article Inflammation Neuroscience

MSC transplantation ameliorates depression in lupus by suppressing Th1 cell–shaped synaptic stripping

Abstract

Systemic lupus erythematosus (SLE), an autoimmune disease, can cause psychiatric disorders, particularly depression, via immune activation. Human umbilical cord mesenchymal stromal cell (hUCMSC) transplantation (MSCT) has been shown to ameliorate immune dysfunction in SLE by inducing immune tolerance. However, whether MSCT can relieve the depressive symptoms in SLE remains incompletely understood. Here, we demonstrate that MSCT relieved early-onset depression-like behavior in both genetically lupus-prone (MRL/lpr) and pristane-induced lupus mice by rescuing impaired hippocampal synaptic connectivity. Transplanted hUCMSCs targeted Th1 cell–derived IFN-γ to inhibit neuronal JAK/STAT1 signaling and downstream CCL8 expression, reducing phagocytic microglia apposition to alleviate synaptic engulfment and neurological dysfunction in young (8-week-old) lupus mice. Systemic delivery of exogenous IFN-γ blunted MSCT-mediated alleviation of synaptic loss and depressive behavior in lupus mice, suggesting that the IFN-γ/CCL8 axis may be an effective therapeutic target and that MSCT is a potential therapy for lupus-related depression. In summary, transplanted hUCMSCs can target systemic immunity to ameliorate psychiatric disorders by rescuing synaptic loss, highlighting the active role of neurons as intermediaries between systemic immunity and microglia in this process.

Authors

Xiaojuan Han, Dandan Wang, Liang Chen, Hua Song, Xiulan Zheng, Xin Zhang, Shengnan Zhao, Jun Liang, Tianshu Xu, Zhibin Hu, Lingyun Sun

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Figure 6

Patients with SLE showed activation of the IFN-γ/JAK/STAT pathway and elevated CCL8 levels in CSF.

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Patients with SLE showed activation of the IFN-γ/JAK/STAT pathway and el...
(A) ELISA revealed that patients with SLE (n = 15) had higher serum levels of IFN-γ than normal controls did (n = 11). (B) Flow cytometric analysis revealed that the number of CD4+IFN-γ+ cells in the peripheral blood was greater in patients with SLE (n = 15) than in normal controls (n = 11). (C and D) qPCR analysis showing the levels of IFNG and IFITM3 in sorted CD4+ T cells from patients with SLE (n = 15) and normal controls (n = 11). (E) Western blot analysis revealed that p-JAK1, p-JAK2, and p-STAT1 levels were increased in CD4+ T cells from patients with SLE. (F) Protein levels of IFN-γ in the cultured supernatants of CD4+ T cells cocultured with/without MSCs under Th1-polarizing conditions for 5 days (n = 5). (G and H) IFN-γ and CCL8 levels in CSF samples from controls (n = 6), non-NPSLE patients (n = 9), and NPSLE patients (n = 14). (I) Analysis of the correlation between CCL8 levels in the CSF and SLEDAI scores in patients with SLE (n = 23). The data are presented as mean ± SEM. *P < 0.05; **P < 0.01; ***P < 0.001, determined using 2-tailed unpaired t test (A-D and F), or 1-way ANOVA followed by Sidak’s post hoc test (G and H). NS, not significant. The correlation coefficient r and P values were calculated via Spearman’s r test in I. SLEDAI, System Lupus Erythematosus Disease Activity Index. See also Supplemental Figure 11.