4.7 Article

Global research trends of Apolipoprotein E in central nervous system: A scientometric analysis

期刊

INTERNATIONAL IMMUNOPHARMACOLOGY
卷 98, 期 -, 页码 -

出版社

ELSEVIER
DOI: 10.1016/j.intimp.2021.107919

关键词

Scientometric analysis; apolipoprotein E; Central nervous system; Neuroinflammation; Inflammasome

资金

  1. National Natural Science Founda-tion of China [81901270, 82072229]

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The research on APOE in CNS is not trendy over the past two decades, despite the involvement of numerous funds, organizations, and scholars. There is a lack of close cooperation between top teams in this field and others worldwide. New ideas may reignite scholars' interest in studying APOE in CNS, with a potential focus on the crosstalk between ApoE and inflammasome in future research.
Apolipoprotein E (apoE, protein; APOE, gene) involves in cholesterol recycling and redistribution by mediating lipoprotein pathways unique to central nervous system (CNS), which is a potential therapeutic target for diseases. We visually analyzed the research hotspots of APOE related to CNS in this work, by scientometric analysis from the Web of Science Core Collection (WOSCC) database over the past two decades. A total of 25,719 references of APOE and 836 references of APOE in CNS were retrieved from the WOSCC on October 26, 2020, and then VOSviewer 1.6.15, Citespace 5.7.R2 were used for visual analysis. Over the last two decades, the research on the field of APOE in CNS is not faddish. Although many funds, organizations, and scholars were affiliated in this field, organizations and scholars, especially the top teams in this field, still lacked close cooperation with other teams around the world. Few articles with high citations had been published in the last decade, but recent studies still lacked scale and breakthrough, and the keywords associated with APOE appeared more outdated. However, the current researches have not fully elucidated the crosstalk between APOE and neuroinflammation in CNS, some new ideas may rekindle the research enthusiasm of scholars. Although the field of APOE in CNS appeared more outdated. Based on keyword analysis, we hypothesized new ideas for further investigation of neuroinflammation would light the interest of APOE in CNS for the scholars. The crosstalk between ApoE and inflammasome may be the focus of future researches. How APOE modulates the time course or intensity of the inflammasome activation, inflammatory response (proinflammatory or anti-inflammatory), and pathological process of CNS disease deserves future attention in both basic and clinical studies. More apoE/APOE-targeted pharmacological interventions will be available for preclinical experiments and clinical trials and bring hope for patients with CNS diseases.

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