Publication Name	World Journal of Diabetes
Manuscript ID	80304
Country	China

Received	2022-09-22 07:50
Peer-Review Started	2022-09-22 07:54
To Make the First Decision
Return for Revision	2022-12-26 08:27
Revised	2023-01-08 13:36
Second Decision	2023-02-15 03:52
Accepted by Journal Editor-in-Chief
Accepted by Company Editor-in-Chief	2023-02-15 21:07
Articles in Press	2023-02-15 21:07
Publication Fee Transferred
Edit the Manuscript by Language Editor
Typeset the Manuscript	2023-03-09 11:06
Publish the Manuscript Online	2023-03-15 15:41

ISSN	1948-9358 (online)
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Category	Cell Biology
Manuscript Type	Basic Study
Article Title	Nε-(carboxymethyl)lysine promotes lipid uptake of macrophage via cluster of differentiation 36 and receptor for advanced glycation end products
Manuscript Source	Unsolicited Manuscript
All Author List	Zhong-Qun Wang, Hai-Peng Yao and Zhen Sun
ORCID	Author(s) ORCID Number Zhong-Qun Wang http://orcid.org/0000-0003-3590-9313 Zhen Sun http://orcid.org/0000-0003-3368-1976
Funding Agency and Grant Number	Funding Agency Grant Number National Natural Science Foundation of China 82070455 Natural Science Foundation of Jiangsu Province BK20201225 Medical Innovation Team Project of Jiangsu Province CXTDA2017010
Corresponding Author	Zhen Sun, PhD, Doctor, Department of Cardiology, Affiliated Hospital of Jiangsu University, No. 438 Jiefang Road, Zhenjiang 212001, Jiangsu Province, China. 1398041019@qq.com
Key Words	Nε-(carboxymethyl)lysine; Cluster of differentiation 36; Receptor for advanced glycation end products; Lipid uptake; Macrophage
Core Tip	Nε-(carboxymethyl)lysine (CML), a toxic metabolism product in diabetes mellites, is a causative factor of many diseases. CML has been reported to promote lipid uptake in macrophages and foam cell formation. The receptor for advanced glycation end products (RAGE) and cluster of differentiation 36 (CD36) are receptors of CML. However, the roles of RAGE and CD36 in CML-induced lipid uptake in macrophages are currently unclear. Moreover, the relationship and difference between RAGE and CD36 in this process are also worth exploring. The in vitro model was constructed with Raw264.7 cells. Under the stimulation of CML, the lipid uptake by cells was significantly increased. Inhibition of CD36 or RAGE antagonized CML-induced lipid uptake. We synthesized a probe of 18F-CML to explore the relationship of CML to CD36 and to RAGE. CML could bind to CD36 and to RAGE, and CML has a significantly stronger affinity for CD36 than for RAGE. The exploration of the pathogenic mechanism of CML may provide evidence for a deeper understanding of diseases related to metabolic disorders.
Publish Date	2023-03-15 15:41
Citation	Wang ZQ, Yao HP, Sun Z. Nε-(carboxymethyl)lysine promotes lipid uptake of macrophage via cluster of differentiation 36 and receptor for advanced glycation end products. World J Diabetes 2023; 14(3): 222-233
URL	https://www.wjgnet.com/1948-9358/full/v14/i3/222.htm
DOI	https://dx.doi.org/10.4239/wjd.v14.i3.222

Full Article (PDF)	WJD-14-222.pdf
Full Article (Word)	WJD-14-222.docx
Manuscript File	80304_Auto_Edited-LM.docx
Answering Reviewers	80304-Answering reviewers.pdf
Audio Core Tip	80304-Audio core tip.mp3
Biostatistics Review Certificate	80304-Biostatistics statement.pdf
Conflict-of-Interest Disclosure Form	80304-Conflict-of-interest statement.pdf
Copyright License Agreement	80304-Copyright license agreement.pdf
Approved Grant Application Form(s) or Funding Agency Copy of any Approval Document(s)	80304-Grant application form(s).pdf
Institutional Animal Care and Use Committee Approval Form or Document	80304-Institutional Animal Care and Use Committee Approval Form or Document.pdf
Institutional Review Board Approval Form or Document	80304-Institutional review board statement.pdf
Non-Native Speakers of English Editing Certificate	80304-Language certificate.pdf
Peer-review Report	80304-Peer-review(s).pdf
Scientific Misconduct Check	80304-Bing-Liu GL-2.png
Scientific Editor Work List	80304-Scientific editor work list.pdf