Clinical and Developmental Immunology (Jan 2012)

Phenotyping of P105-Negative B Cell Subsets in Patients with Systemic Lupus Erythematosus

  • Syuichi Koarada,
  • Yoshifumi Tada,
  • Rie Suematsu,
  • Sachiko Soejima,
  • Hisako Inoue,
  • Akihide Ohta,
  • Kohei Nagasawa

DOI
https://doi.org/10.1155/2012/198206
Journal volume & issue
Vol. 2012

Abstract

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This study aimed to investigate phenotype of RP105(−) B cell subsets in patients with systemic lupus erythematosus (SLE). Flow cytometry was used for phenotyping RP105-negaive B cell subsets. Based on CD19, RP105, and CD138 expression, RP105(−) B cells consist of at least 5 subsets of late B cells, including CD19(+)RP105(int), CD19(+) RP105(−), CD19(low) RP105(−) CD138(−), CD19(low) RP105(−)CD138(int), and CD19(low) RP105(−) CD138(++) B cells. Especially, CD19(+)RP105(int) and CD19(low) RP105(−)CD138(int) B cells are significantly larger than other RP105(−) B cell subsets in SLE. By comparison of RP105(−) B cell subsets between patients with SLE and normal subjects, these subsets were detectable even in normal subjects, but the percentages of RP105(−) B cell subsets were significantly larger in SLE. The phenotypic analysis of RP105(−) B cell subsets suggests dysregulation of later B cell subsets in SLE and may provide new insights into understanding regulation of B cells in human SLE.