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首页> 外文期刊>The Journal of investigative dermatology. >Pro-Inflammatory Chemokines and Cytokines Dominate the Blister Fluid Molecular Signature in Patients with Epidermolysis Bullosa and Affect Leukocyte and Stem Cell Migration
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Pro-Inflammatory Chemokines and Cytokines Dominate the Blister Fluid Molecular Signature in Patients with Epidermolysis Bullosa and Affect Leukocyte and Stem Cell Migration

机译:促炎趋化因子和细胞因子在表皮分解患者患者中占主导地位,并影响白细胞和干细胞迁移

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摘要

Hereditary epidermolysis bullosa (EB) is associated with skin blistering and the development of chronic nonhealing wounds. Although clinical studies have shown that cell-based therapies improve wound healing, the recruitment of therapeutic cells to blistering skin and to more advanced skin lesions remains a challenge. Here, we analyzed cytokines and chemokines in blister fluids of patients affected by dystrophic, junctional, and simplex EB. Our analysis revealed high levels of CXCR1, CXCR2, CCR2, and CCR4 ligands, particularly dominant in dystrophic and junctional EB. In?vitro migration assays demonstrated the preferential recruitment of CCR4 + lymphocytes and CXCR1 + , CXCR2 + , and CCR2 + myeloid cells toward EB-derived blister fluids. Immunophenotyping of skin-infiltrating leukocytes confirmed substantial infiltration of EB-affected skin with resting (CD45RA + ) and activated (CD45RO + ) T cells and CXCR2 + CD11b + cells, many of which were identified as CD16b + neutrophils. Our studies also showed that abundance of CXCR2 ligand in blister fluids also creates a favorable milieu for the recruitment of the CXCR2 + stem cells, as validated by in?vitro and in-matrix migration assays. Collectively, this study identified several chemotactic pathways that control the recruitment of leukocytes to the EB-associated skin lesions. These chemotactic axes could be explored for the refinement of the cutaneous homing of the therapeutic stem cells.
机译:遗传性表皮分解Bullosa(EB)与皮肤起泡和慢性非热伤的发育有关。虽然临床研究表明,基于细胞的疗法改善伤口愈合,但招募治疗细胞对皮肤皮肤和更先进的皮肤病变仍然是一个挑战。在这里,我们分析了受营养不良,结和单纯乳头患者影响的患者的水疱流体中的细胞因子和趋化因子。我们的分析显示了高水平的CXCR1,CXCR2,CCR2和CCR4配体,特别是营养不良和结eB中的显性。在体外迁移测定中,证明了对CCR4 +淋巴细胞和CXCR1 +,CXCR2 +和CCR2 +骨髓细胞的优先募集朝向EB衍生的泡罩流体。皮肤渗透白细胞的免疫蛋白酶分型证实了EB受影响的皮肤具有休息(CD45RA +)和活化(CD45RO +)T细胞和CXCR2 + CD11b +细胞的显着渗透,其中许多鉴定为CD16B +中性粒细胞。我们的研究还表明,泡罩流体中的CXCR2配体的丰富也为CXCR2 +干细胞募集的良好的Milieu,如在体外和基质迁移测定中验证。本研究统称,确定了几种趋化途径,可控制白细胞对EB相关皮肤病变的招募。这些趋化轴可以探索用于细化治疗干细胞的皮肤归巢。

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    Department of Dermatology and Cutaneous Biology Jefferson Medical College Thomas Jefferson;

    Department of Basic Sciences Health Sciences Division University of Monterrey;

    Facultad de Medicina Clínica Alemana Universidad del Desarrollo;

    Department of Dermatology and Cutaneous Biology Jefferson Medical College Thomas Jefferson;

    Department of Diagnostic Science Louisiana State University School of Dentistry;

    Department of Dermatology and Cutaneous Biology Jefferson Medical College Thomas Jefferson;

    Department of Dermatology and Cutaneous Biology Jefferson Medical College Thomas Jefferson;

    Department of Dermatology and Cutaneous Biology Jefferson Medical College Thomas Jefferson;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 皮肤病学与性病学;
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