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白细胞介素-8 通过促进淋巴管再生来减少术后淋巴水肿的形成。

Interleukin-8 reduces post-surgical lymphedema formation by promoting lymphatic vessel regeneration.

机构信息

Department of Surgery, Norris Comprehensive Cancer Center, University of Southern California, Los Angeles, CA 90033, USA.

出版信息

Angiogenesis. 2013 Jan;16(1):29-44. doi: 10.1007/s10456-012-9297-6. Epub 2012 Sep 4.

Abstract

Lymphedema is mainly caused by lymphatic obstruction and manifested as tissue swelling, often in the arms and legs. Lymphedema is one of the most common post-surgical complications in breast cancer patients and presents a painful and disfiguring chronic illness that has few treatment options. Here, we evaluated the therapeutic potential of interleukin (IL)-8 in lymphatic regeneration independent of its pro-inflammatory activity. We found that IL-8 promoted proliferation, tube formation, and migration of lymphatic endothelial cells (LECs) without activating the VEGF signaling. Additionally, IL-8 suppressed the major cell cycle inhibitor CDKN1C/p57(KIP2) by downregulating its positive regulator PROX1, which is known as the master regulator of LEC-differentiation. Animal-based studies such as matrigel plug and cornea micropocket assays demonstrated potent efficacy of IL-8 in activating lymphangiogenesis in vivo. Moreover, we have generated a novel transgenic mouse model (K14-hIL8) that expresses human IL-8 in the skin and then crossed with lymphatic-specific fluorescent (Prox1-GFP) mouse. The resulting double transgenic mice showed that a stable expression of IL-8 could promote embryonic lymphangiogenesis. Moreover, an immunodeficient IL-8-expressing mouse line that was established by crossing K14-hIL8 mice with athymic nude mice displayed an enhanced tumor-associated lymphangiogenesis. Finally, when experimental lymphedema was introduced, K14-hIL8 mice showed an improved amelioration of lymphedema with an increased lymphatic regeneration. Together, we report that IL-8 can activate lymphangiogenesis in vitro and in vivo with a therapeutic efficacy in post-surgical lymphedema.

摘要

淋巴水肿主要由淋巴阻塞引起,表现为组织肿胀,常发生在手臂和腿部。淋巴水肿是乳腺癌患者术后最常见的并发症之一,表现为一种痛苦且致残的慢性疾病,治疗选择有限。在这里,我们评估了白细胞介素(IL)-8 在独立于其促炎活性的情况下促进淋巴再生的治疗潜力。我们发现,IL-8 促进淋巴管内皮细胞(LEC)的增殖、管形成和迁移,而不激活 VEGF 信号。此外,IL-8 通过下调其阳性调节剂 PROX1 来抑制主要细胞周期抑制剂 CDKN1C/p57(KIP2),PROX1 被称为 LEC 分化的主调控因子。基于动物的研究,如 Matrigel plugs 和角膜微囊 assay 表明,IL-8 在体内激活淋巴管生成具有强大的功效。此外,我们已经生成了一种新型的转基因小鼠模型(K14-hIL8),该模型在皮肤中表达人 IL-8,然后与淋巴管特异性荧光(Prox1-GFP)小鼠杂交。由此产生的双转基因小鼠表明,IL-8 的稳定表达可以促进胚胎期淋巴管生成。此外,通过将 K14-hIL8 小鼠与无胸腺裸鼠杂交建立的免疫缺陷型 IL-8 表达小鼠系显示出增强的肿瘤相关淋巴管生成。最后,当引入实验性淋巴水肿时,K14-hIL8 小鼠显示出淋巴水肿改善的改善,淋巴管再生增加。总之,我们报告 IL-8 可以在体外和体内激活淋巴管生成,并在术后淋巴水肿中具有治疗功效。

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