Fabre-Mersseman Véronique, Tubiana Roland, Papagno Laura, Bayard Charles, Briceno Olivia, Fastenackels Solène, Dudoit Yasmine, Rostane Hafeda, Salmon Dominique, Costagliola Dominique, Caby Fabienne, Sauce Delphine, Viard Jean-Paul, Appay Victor
aSorbonne Universités, UPMC Univ Paris, Centre d'Immunologie et des Maladies Infectieuses (CIMI-Paris) bINSERM, U1135, CIMI-Paris cSorbonne université, UPMC Univ Paris 06, UMR_S 1136 Pierre Louis Institute of Epidemiology and Public Health dINSERM, UMR_S 1136, Institut Pierre Louis d'Epidémiologie et de Santé Publique eAP-HP, Groupe hospitalier Pitié-Salpêtrière, Service des Maladies Infectieuses et Tropicales fAP-HP, Hôtel-Dieu, Centre de Diagnostic et de Thérapeutique gCochin Hospital, Infectious Pathology Unit, France and Paris Descartes University, Infectious Pathology Unit hEA 7327 Université Paris-Descartes, Sorbonne Paris Cité, Paris, France.
AIDS. 2014 Nov 28;28(18):2677-82. doi: 10.1097/QAD.0000000000000472.
A majority of HIV-1-infected patients present a severe deficit in vitamin D, which predicts short-term mortality. Vitamin D is a naturally synthesized hormone, with important immunomodulatory functions. In the general population, its deficit has been associated with increased markers of inflammation. Vitamin D deficit may therefore play a role in the establishment of elevated systemic immune activation, which persists despite suppressive antiretroviral therapy (ART) in HIV-infected patients, and is predictive of disease progression; and vitamin D supplementation may be beneficial in this context.
We performed both a cross-sectional study (vitamin D deficit versus normal level) and a longitudinal study (upon vitamin D supplementation for 6 to 12 months) of HIV-1-infected patients receiving suppressive ART. The primary outcome measure was the percentage of activated memory CD8(+) T cells in blood, which is a robust marker associated with disease progression. Secondary outcomes included general T-lymphocyte and B-lymphocyte phenotype.
Although vitamin D deficiency had no influence on T-cell and B-cell subset distribution, we found an association between vitamin D and immune activation levels in HIV-1-infected patients. Vitamin D supplementation in vitamin D-deficient patients resulted in reduced immune activation levels.
The present data support the rationale of vitamin D supplementation in the routine clinical management of HIV-1-infected patients, in order to decrease immune activation levels and possibly improve long-term survival.
大多数感染HIV-1的患者存在严重的维生素D缺乏,这预示着短期死亡率。维生素D是一种天然合成的激素,具有重要的免疫调节功能。在普通人群中,其缺乏与炎症标志物增加有关。因此,维生素D缺乏可能在全身免疫激活升高的过程中起作用,这种免疫激活在接受抗逆转录病毒治疗(ART)的HIV感染患者中持续存在,并且是疾病进展的预测指标;在这种情况下补充维生素D可能有益。
我们对接受抑制性ART的HIV-1感染患者进行了一项横断面研究(维生素D缺乏与正常水平对比)和一项纵向研究(补充维生素D 6至12个月)。主要结局指标是血液中活化记忆CD8(+) T细胞的百分比,这是与疾病进展相关的一个可靠标志物。次要结局包括一般T淋巴细胞和B淋巴细胞表型。
尽管维生素D缺乏对T细胞和B细胞亚群分布没有影响,但我们发现维生素D与HIV-1感染患者的免疫激活水平之间存在关联。对维生素D缺乏的患者补充维生素D可降低免疫激活水平。
目前的数据支持在HIV-1感染患者的常规临床管理中补充维生素D的基本原理,以降低免疫激活水平并可能改善长期生存。
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