Characteristics and impact of infiltration of B-cells from systemic sclerosis patients in a 3D healthy skin model

Mathilde Le Maître, T. Guerrier, A. Collet, M. Derhourhi, Jean-Pascal Meneboo, B. Toussaint, Amélie Bonnefond, C. Villenet, Shéhérazade Sebda, Antonino Bongiovanni, Meryem Tardivel, Myriam Simon, M. Jendoubi, Blanche Daunou, Alexis Largy, M. Figeac, Sylvain Dubucquoi, David Launay
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Abstract

In systemic sclerosis (SSc), B-cells are activated and present in the skin and lung of patients where they can interact with fibroblasts. The precise impact and mechanisms of the interaction of B-cells and fibroblasts at the tissular level are poorly studied.We investigated the impact and mechanisms of B-cell/fibroblast interactions in cocultures between B-cells from patients with SSc and 3-dimensional reconstituted healthy skin model including fibroblasts, keratinocytes and extracellular matrix.The quantification and description of the B-cell infiltration in 3D cocultures were performed using cells imagery strategy and cytometry. The effect of coculture on the transcriptome of B-cells and fibroblasts was studied with bulk and single-cell RNA sequencing approaches. The mechanisms of this interaction were studied by blocking key cytokines like IL-6 and TNF.We showed a significant infiltration of B-cells in the 3D healthy skin model. The amount but not the depth of infiltration was higher with B-cells from SSc patients and with activated B-cells. B-cell infiltrates were mainly composed of naïve and memory cells, whose frequencies differed depending on B-cells origin and activation state: infiltrated B-cells from patients with SSc showed an activated profile and an overexpression of immunoglobulin genes compared to circulating B-cells before infiltration. Our study has shown for the first time that activated B-cells modified the transcriptomic profile of both healthy and SSc fibroblasts, toward a pro-inflammatory (TNF and IL-17 signaling) and interferon profile, with a key role of the TNF pathway.B-cells and 3D skin cocultures allowed the modelization of B-cells infiltration in tissues observed in SSc, uncovering an influence of the underlying disease and the activation state of B-cells. We showed a pro-inflammatory effect on skin fibroblasts and pro-activation effect on infiltrating B-cells during coculture. This reinforces the role of B-cells in SSc and provide potential targets for future therapeutic approach in this disease.
三维健康皮肤模型中系统性硬化症患者 B 细胞浸润的特征和影响
系统性硬化症(SSc)患者的皮肤和肺部存在活化的 B 细胞,它们可以与成纤维细胞相互作用。我们研究了系统性硬化症患者的 B 细胞与包括成纤维细胞、角质细胞和细胞外基质在内的三维重建健康皮肤模型共培养中 B 细胞/成纤维细胞相互作用的影响和机制。通过大量和单细胞 RNA 测序方法研究了共培养对 B 细胞和成纤维细胞转录组的影响。通过阻断 IL-6 和 TNF 等关键细胞因子,研究了这种相互作用的机制。来自 SSc 患者的 B 细胞和活化 B 细胞的浸润量更高,但浸润深度却不高。B细胞浸润主要由幼稚细胞和记忆细胞组成,其频率因B细胞来源和活化状态而异:与浸润前的循环B细胞相比,SSc患者的浸润B细胞显示出活化特征和免疫球蛋白基因的过度表达。我们的研究首次表明,活化的B细胞改变了健康和SSc成纤维细胞的转录组特征,使其趋向于促炎(TNF和IL-17信号)和干扰素特征,其中TNF通路起着关键作用。B细胞和三维皮肤共培养物可模拟B细胞在SSc组织中的浸润,揭示潜在疾病和B细胞活化状态的影响。在共培养过程中,我们发现了对皮肤成纤维细胞的促炎作用和对浸润的 B 细胞的促活化作用。这加强了 B 细胞在 SSc 中的作用,并为该疾病的未来治疗方法提供了潜在靶点。
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