Radiation Impacts Early Atherosclerosis by Suppressing Intimal LDL Accumulation

Author:

Ikeda Jiro12ORCID,Scipione Corey A.123ORCID,Hyduk Sharon J.1,Althagafi Marwan G.12,Atif Jawairia143ORCID,Dick Sarah A.14235ORCID,Rajora Maneesha6,Jang Erika27ORCID,Emoto Takuo1,Murakami Junichi18ORCID,Ikeda Noriko1ORCID,Ibrahim Hisham M.12ORCID,Polenz Chanele K.12,Gao Xiaotang1,Tai Kelly13,Jongstra-Bilen Jenny123,Nakashima Ryota6ORCID,Epelman Slava19235,Robbins Clinton S.1923,Zheng Gang6,Lee Warren L.2107ORCID,MacParland Sonya A.123ORCID,Cybulsky Myron I.1923ORCID

Affiliation:

1. Toronto General Hospital Research Institute (J.I., C.A.S., S.J.H., M.G.A., J.A., S.A.D., T.E., J.M., N.I., H.M.I., C.K.P., X.G., K.T., J.J.-B., S.E., C.S.R., S.A.M., M.I.C.), University Health Network, Toronto, Canada.

2. Laboratory Medicine and Pathobiology (J.I., C.A.S., M.G.A., E.J., H.M.I., C.K.P., J.J.-B., S.E., C.S.R., W.L.L., S.A.M., M.I.C.), University of Toronto.

3. Immunology (C.A.S., J.A., S.A.D., K.T., J.J.-B., S.E., C.S.R., S.A.M., M.I.C.), University of Toronto.

4. Ajmera Family Transplant Centre, Toronto General Hospital Research Institute (J.A., S.A.M.), University Health Network, Toronto, Canada.

5. Ted Rogers Centre for Heart Research, Translational Biology and Engineering Program (S.A.D., S.E.).

6. Princess Margaret Cancer Centre (M.R., R.N., G.Z.), University Health Network, Toronto, Canada.

7. Keenan Research Centre, Unity Health (E.J., W.L.L.).

8. Latner Thoracic Surgery Research Laboratories (J.M.), University Health Network, Toronto, Canada.

9. Peter Munk Cardiac Centre (S.E., C.S.R., M.I.C.), University Health Network, Toronto, Canada.

10. Medicine (W.L.L.), University of Toronto.

Abstract

Rationale: Bone marrow transplantation (BMT) is used frequently to study the role of hematopoietic cells in atherosclerosis, but aortic arch lesions are smaller in mice after BMT. Objective: To identify the earliest stage of atherosclerosis inhibited by BMT and elucidate potential mechanisms. Methods and Results: Ldlr −/− mice underwent total body γ-irradiation, bone marrow reconstitution, and 6-week recovery. Atherosclerosis was studied in the ascending aortic arch and compared with mice without BMT. In BMT mice, neutral lipid and myeloid cell topography were lower in lesions after feeding a cholesterol-rich diet for 3, 6, and 12 weeks. Lesion coalescence and height were suppressed dramatically in mice post-BMT, whereas lateral growth was inhibited minimally. Targeted radiation to the upper thorax alone reproduced the BMT phenotype. Classical monocyte recruitment, intimal myeloid cell proliferation, and apoptosis did not account for the post-BMT phenotype. Neutral lipid accumulation was reduced in 5-day lesions, thus we developed quantitative assays for LDL (low-density lipoprotein) accumulation and paracellular leakage using DiI-labeled human LDL and rhodamine B-labeled 70 kD dextran. LDL accumulation was dramatically higher in the intima of Ldlr −/− relative to Ldlr +/+ mice, and was inhibited by injection of HDL mimics, suggesting a regulated process. LDL, but not dextran, accumulation was lower in mice post-BMT both at baseline and in 5-day lesions. Since the transcript abundance of molecules implicated in LDL transcytosis was not significantly different in the post-BMT intima, transcriptomics from whole aortic arch intima, and at single-cell resolution, was performed to give insights into pathways modulated by BMT. Conclusions: Radiation exposure inhibits LDL entry into the aortic intima at baseline and the earliest stages of atherosclerosis. Single-cell transcriptomic analysis suggests that LDL uptake by endothelial cells is diverted to lysosomal degradation and reverse cholesterol transport pathways. This reduces intimal accumulation of lipid and impacts lesion initiation and growth.

Funder

Gouvernement du Canada | Canadian Institutes of Health Research

Gouvernement du Canada | CIHR | Institute of Infection and Immunity

Heart and Stroke Foundation of Canada

Gouvernement du Canada | CIHR | Institute of Circulatory and Respiratory Health

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine,Physiology

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