I型巨噬细胞清道夫受体的失活促进载脂蛋白E缺陷小鼠动脉粥样硬化病变的发展。
Inactivation of macrophage scavenger receptor class B type I promotes atherosclerotic lesion development in apolipoprotein E-deficient mice.
作者信息
Zhang Wenwu, Yancey Patricia G, Su Yan Ru, Babaev Vladimir R, Zhang Yuomin, Fazio Sergio, Linton MacRae F
机构信息
Atherosclerosis Research Unit, Division of Cardiovascular Medicine, Departments of Medicine, Vanderbilt University Medical Center, Nashville, Tenn 37232-6300, USA.
出版信息
Circulation. 2003 Nov 4;108(18):2258-63. doi: 10.1161/01.CIR.0000093189.97429.9D. Epub 2003 Oct 27.
BACKGROUND
Scavenger receptor class B type I (SR-BI) is expressed in macrophages, where it has been proposed to facilitate cholesterol efflux. However, direct evidence that the expression of macrophage SR-BI is protective against atherosclerosis is lacking. In this study, we examined the in vivo role of macrophage SR-BI in atherosclerotic lesion development in the apolipoprotein (apo) E-deficient mouse model.
METHODS AND RESULTS
ApoE-deficient mice with (n=16) or without (n=15) expression of macrophage SR-BI were created by transplanting lethally irradiated apoE-deficient mice with bone marrow cells collected from SR-BI-/- apoE-/- mice or SR-BI+/+ apoE-/- mice. The recipient mice were fed a chow diet for 12 weeks after transplantation for analysis of atherosclerosis. Quantification of macrophage SR-BI mRNA by real-time reverse transcription-polymerase chain reaction indicated successful engraftment of donor bone marrow and inactivation of macrophage SR-BI in recipient mice reconstituted with SR-BI-/- apoE-/- bone marrow. There were no significant differences in plasma lipid levels, lipoprotein distributions, and HDL subpopulations between the 2 groups. Analysis of the proximal aorta demonstrated an 86% increase in mean atherosclerotic lesion area in SR-BI-/- apoE-/- --> apoE-/- mice compared with SR-BI+/+ apoE-/- --> apoE-/- mice (109.50+/-18.08 versus 58.75+/-9.58x10(3) microm2; mean+/-SEM, P=0.017). No difference in cholesterol efflux from SR-BI+/+ apoE-/- or SR-BI-/- apoE-/- macrophages to HDL or apoA-I discs was detected.
CONCLUSIONS
Expression of macrophage SR-BI protects mice against atherosclerotic lesion development in apoE-deficient mice in vivo without influencing plasma lipids, HDL subpopulations, or cholesterol efflux. Thus, macrophage SR-BI plays an antiatherogenic role in vivo, providing a new therapeutic target for the design of strategies to prevent and treat atherosclerosis.
背景
I 型 B 类清道夫受体(SR-BI)在巨噬细胞中表达,有人提出它可促进胆固醇外流。然而,缺乏巨噬细胞 SR-BI 表达对动脉粥样硬化具有保护作用的直接证据。在本研究中,我们在载脂蛋白(apo)E 缺陷小鼠模型中研究了巨噬细胞 SR-BI 在动脉粥样硬化病变发展中的体内作用。
方法与结果
通过将经致死剂量照射的 apoE 缺陷小鼠与从 SR-BI-/- apoE-/- 小鼠或 SR-BI+/+ apoE-/- 小鼠收集的骨髓细胞进行移植,创建了有(n = 16)或无(n = 15)巨噬细胞 SR-BI 表达的 apoE 缺陷小鼠。移植后,给受体小鼠喂食普通饲料 12 周以分析动脉粥样硬化。通过实时逆转录 - 聚合酶链反应对巨噬细胞 SR-BI mRNA 进行定量分析表明,在用 SR-BI-/- apoE-/- 骨髓重建的受体小鼠中,供体骨髓成功植入且巨噬细胞 SR-BI 失活。两组之间的血浆脂质水平、脂蛋白分布和高密度脂蛋白亚群无显著差异。对主动脉近端的分析表明,与 SR-BI+/+ apoE-/-→apoE-/- 小鼠相比,SR-BI-/- apoE-/-→apoE-/- 小鼠的平均动脉粥样硬化病变面积增加了 86%(109.50±18.08 对 58.75±9.58x10(3) 平方微米;平均值±标准误,P = 0.017)。未检测到 SR-BI+/+ apoE-/- 或 SR-BI-/- apoE-/- 巨噬细胞向高密度脂蛋白或载脂蛋白 A-I 圆盘的胆固醇外流存在差异。
结论
巨噬细胞 SR-BI 的表达可保护小鼠在体内免受 apoE 缺陷小鼠动脉粥样硬化病变的发展,而不影响血浆脂质、高密度脂蛋白亚群或胆固醇外流。因此,巨噬细胞 SR-BI 在体内发挥抗动脉粥样硬化作用,为预防和治疗动脉粥样硬化策略的设计提供了新的治疗靶点。
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