Frontiers in Medicine (Apr 2022)

Bibliometric Analysis of Birt-Hogg-Dubé Syndrome From 2001 to 2021

  • Shixu Liu,
  • Shixu Liu,
  • Kun Xia,
  • Xiaohong Liu,
  • Xiaohong Liu,
  • Yuanyuan Duan,
  • Mu Hu,
  • Mu Hu,
  • Hongsheng Xia,
  • Jiayu Lv,
  • Jiayu Lv,
  • Lili Zhang,
  • Lili Zhang,
  • Yanyi Liu,
  • Yanyi Liu,
  • Xiao Xia,
  • Xiao Xia,
  • Guangxi Li,
  • Xiangning Cui

DOI
https://doi.org/10.3389/fmed.2022.857127
Journal volume & issue
Vol. 9

Abstract

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BackgroundBirt-Hogg-Dubé syndrome (BHD) is a rare autosomal dominant inherited disorder caused by germline mutations in folliculin (FLCN). Despite our significantly evolved understanding of BHD over the past decades, no bibliometric analyses have been conducted in this field. This study aimed to analyze and visualize the characteristics of publication outputs, the research hotspots, and scientific frontiers about BHD using bibliometric analysis.MethodsAll relevant literature on BHD was culled from the Web of Science Core Collection (WoSCC) database. Valid data were extracted from the articles and visually analyzed using CiteSpace and VOSviewer.ResultsA total of 751 qualifying papers were included. Publication outputs concerning BHD increased over time. The dominant position of the United States and Japan in BHD research field was evident. National Cancer Institute (the USA) and Yokohama City University (Japan) were the two most productive organizations. W. Marston Linehan exerted a considerable publication impact and had made the most remarkable contributions in the field of BHD. Plos One was the journal with the highest publication outputs, and half of the top 10 journals and co-cited journals belonged to Q1 or Q2. Keyword citation bursts revealed that management, tumor suppressor, flcn gene, spectrum, diagnosis, risk, computed tomography were the emerging research hotspots.ConclusionResearch on BHD is prosperous. International cooperation between countries and organizations is also expected to deepen and strengthen in the future. Our results indicated that FLCN-associated pathways involved in the pathogenesis of BHD, specific options for early diagnosis, and molecular-targeting therapies will remain research hotspots in the future.

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