Increased infiltration of CD4+ T cell in the complement deficient lymphedema model.

IF 2.9 4区 医学 Q3 IMMUNOLOGY
Toshihiko Nishioka, Kei-Ichi Katayama, Shinji Kumegawa, Kyoichi Isono, Takashi Baba, Hiroshi Tsujimoto, Gen Yamada, Norimitsu Inoue, Shinichi Asamura
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引用次数: 0

Abstract

Background: Lymphedema is an intractable disease that can be caused by injury to lymphatic vessels, such as by surgical treatments for cancer. It can lead to impaired joint mobility in the extremities and reduced quality of life. Chronic inflammation due to infiltration of various immune cells in an area of lymphedema is thought to lead to local fibrosis, but the molecular pathogenesis of lymphedema remains unclear. Development of effective therapies requires elucidation of the immunological mechanisms involved in the progression of lymphedema. The complement system is part of the innate immune system which has a central role in the elimination of invading microbes and acts as a scavenger of altered host cells, such as apoptotic and necrotic cells and cellular debris. Complement-targeted therapies have recently been clinically applied to various diseases caused by complement overactivation. In this context, we aimed to determine whether complement activation is involved in the development of lymphedema.

Results: Our mouse tail lymphedema models showed increased expression of C3, and that the classical or lectin pathway was locally activated. Complement activation was suggested to be involved in the progression of lymphedema. In comparison of the C3 knockout (KO) mouse lymphedema model and wild-type mice, there was no difference in the degree of edema at three weeks postoperatively, but the C3 KO mice had a significant increase of TUNEL+ necrotic cells and CD4+ T cells. Infiltration of macrophages and granulocytes was not significantly elevated in C3 KO or C5 KO mice compared with in wild-type mice. Impaired opsonization and decreased migration of macrophages and granulocytes due to C3 deficiency should therefore induce the accumulation of dead cells and may lead to increased infiltration of CD4+ T cells.

Conclusions: Vigilance for exacerbation of lymphedema is necessary when surgical treatments have the potential to injure lymphatic vessels in patients undergoing complement-targeted therapies or with complement deficiency. Future studies should aim to elucidate the molecular mechanism of CD4+ T cell infiltration by accumulated dead cells.

补体缺乏型淋巴水肿模型中CD4+T细胞浸润增加。
背景:淋巴水肿是一种棘手的疾病,可由淋巴管损伤引起,如癌症的外科治疗。它会导致四肢关节活动能力受损,生活质量下降。淋巴水肿区域各种免疫细胞浸润引起的慢性炎症被认为会导致局部纤维化,但淋巴水肿的分子发病机制尚不清楚。开发有效的治疗方法需要阐明淋巴水肿进展的免疫机制。补体系统是先天免疫系统的一部分,在消除入侵微生物方面发挥核心作用,并作为改变的宿主细胞(如凋亡和坏死细胞以及细胞碎片)的清除剂。补体靶向治疗最近已在临床上应用于由补体过度激活引起的各种疾病。在这种情况下,我们旨在确定补体激活是否参与淋巴水肿的发展。结果:我们的小鼠尾部淋巴水肿模型显示C3的表达增加,并且经典或凝集素途径被局部激活。补体激活被认为与淋巴水肿的进展有关。与C3敲除(KO)小鼠淋巴水肿模型和野生型小鼠相比,术后三周的水肿程度没有差异,但C3敲除小鼠的TUNEL+坏死细胞和CD4+T细胞显著增加。与野生型小鼠相比,C3 KO或C5 KO小鼠中巨噬细胞和粒细胞的浸润没有显著升高。因此,C3缺乏导致的巨噬细胞和粒细胞的调理作用受损和迁移减少应诱导死细胞的积累,并可能导致CD4+T细胞的浸润增加。结论:当接受补体靶向治疗或补体缺乏患者的手术治疗可能损伤淋巴管时,有必要警惕淋巴水肿的恶化。未来的研究应旨在阐明CD4+T细胞通过积累的死细胞浸润的分子机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
BMC Immunology
BMC Immunology 医学-免疫学
CiteScore
5.50
自引率
0.00%
发文量
54
审稿时长
1 months
期刊介绍: BMC Immunology is an open access journal publishing original peer-reviewed research articles in molecular, cellular, tissue-level, organismal, functional, and developmental aspects of the immune system as well as clinical studies and animal models of human diseases.
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