血小板反应蛋白-2 通过激活调节性 T 细胞来预防病毒性心肌炎中的心脏损伤和功能障碍。

Thrombospondin-2 prevents cardiac injury and dysfunction in viral myocarditis through the activation of regulatory T-cells.

机构信息

Department of Cardiology, Center for Heart Failure Research, CARIM, Maastricht University, The Netherlands.

出版信息

Cardiovasc Res. 2012 Apr 1;94(1):115-24. doi: 10.1093/cvr/cvs077. Epub 2012 Feb 2.

DOI:10.1093/cvr/cvs077

PMID:22308237

Abstract

AIMS

Thrombospondin-2 (TSP-2) modulates matrix integrity and myocyte survival in the hypertensive or ageing heart. Whether TSP-2 may affect cardiac inflammation and injury, in particular during acute viral myocarditis, is completely unknown.

METHODS AND RESULTS

Therefore, mortality, cardiac inflammation, and function were assessed in TSP-2-null (KO) and wild-type (WT) mice in human Coxsackie virus B3 (CVB3)-induced myocarditis. TSP-2 KO had an increased mortality when compared with WT mice during viral myocarditis. The absence of TSP-2 resulted in increased cardiac inflammation and injury at 14 days, which resulted in depressed systolic function [fractional shortening (FS); 34 ± 2.6 in WT vs. 24 ± 1.8 in KO mice, P< 0.05] and increased cardiac dilatation (end-diastolic dimensions, mm; 3.7 ± 0.09 in WT vs. 4.8 ± 0.06 in KO mice, P< 0.05) 35 days post-infection. Lack of TSP-2 resulted in a decreased activation of the anti-inflammatory T-regulatory cells, as indicated by a lower number of CD25-positive T-cells, and significantly decreased gene expression of regulatory T-cell markers, Foxp3 and CTLA-4. Finally, overexpression of TSP-2 in WT hearts using cardiotropic vectors derived from adeno-associated virus serotype 9 (AAV9) inhibited cardiac inflammation and injury at 14 days and improved cardiac function at 35 days post-CVB3 infection when compared with control AAV9.

CONCLUSION

TSP-2 has a protective role against cardiac inflammation, injury, and dysfunction in acute viral myocarditis.

摘要

目的

血小板反应蛋白-2（TSP-2）调节高血压或衰老心脏中的基质完整性和心肌细胞存活。TSP-2 是否会影响心脏炎症和损伤，特别是在急性病毒性心肌炎期间，目前尚完全不清楚。

方法和结果

因此，在柯萨奇病毒 B3（CVB3）诱导的心肌炎中，评估了 TSP-2 敲除（KO）和野生型（WT）小鼠的死亡率、心脏炎症和功能。与 WT 小鼠相比，TSP-2 KO 在病毒性心肌炎期间的死亡率增加。TSP-2 的缺失导致 14 天时心脏炎症和损伤增加，导致收缩功能降低[分数缩短（FS）；WT 小鼠为 34±2.6，KO 小鼠为 24±1.8，P<0.05]和心脏扩张增加（舒张末期尺寸，mm；WT 小鼠为 3.7±0.09，KO 小鼠为 4.8±0.06，P<0.05）35 天后感染。缺乏 TSP-2 导致抗炎性 T 调节细胞的激活减少，表现为 CD25 阳性 T 细胞数量减少，以及调节性 T 细胞标记物 Foxp3 和 CTLA-4 的基因表达显著降低。最后，使用源自腺相关病毒血清型 9（AAV9）的心脏靶向载体在 WT 心脏中过表达 TSP-2，与对照 AAV9 相比，可在 14 天时抑制心脏炎症和损伤，并在 CVB3 感染后 35 天时改善心脏功能。

结论

TSP-2 在急性病毒性心肌炎中对心脏炎症、损伤和功能障碍具有保护作用。

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血小板反应蛋白-2 通过激活调节性 T 细胞来预防病毒性心肌炎中的心脏损伤和功能障碍。

Thrombospondin-2 prevents cardiac injury and dysfunction in viral myocarditis through the activation of regulatory T-cells.

机构信息

出版信息

AIMS

METHODS AND RESULTS

CONCLUSION

目的

方法和结果

结论

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