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Stereotyped subset #1 chronic lymphocytic leukemia: A direct link between B-cell receptor structure, function, and patients' prognosis

  • Ilaria Del Giudice
  • , Sabina Chiaretti
  • , Simona Santangelo
  • , Simona Tavolaro
  • , Nadia Peragine
  • , Marilisa Marinelli
  • , Caterina Ilari
  • , Sara Raponi
  • , Monica Messina
  • , Mauro Nanni
  • , Francesca Romana Mauro
  • , Alfonso Piciocchi
  • , Katia Bontempi
  • , Davide Rossi
  • , Gianluca Gaidano
  • , Anna Guarini
  • , Robin Foà

Research output: Contribution to journalArticlepeer-review

Abstract

Chronic lymphocytic leukemia (CLL) with stereotyped B-cell receptor (BCR) belonging to subset #1 (IGHV1-5-7/IGKV1-39) display a poor outcome. To characterize their genetic and genomic features and BCR function, we selected 20 subset #1 CLL from a series of 579 cases. Subset #1 CLL, all showing unmutated IGHV, were associated with the presence of del(11q) (50%) in comparison with unmutated CLL, unmutated stereotyped CLL other than subset #1 and with cases using the same IGHV genes but a heterogeneous VH CDR3 (non-subset #1 CLL). There were no distinctive features regarding CD38, ZAP-70, and TP53 disruption. NOTCH1, SF3B1, and BIRC3 were mutated in 15%, 0%, and 5% of cases, respectively, while BIRC3 was deleted in 22% of cases. Microarray unsupervised analysis on 80 unmutated/mutated/stereotyped/non-stereotyped CLL showed a tight clustering of subset #1 cases. Their genomic signature exhibited several differentially expressed transcripts involved in BCR signal transduction, apoptosis regulation, cell proliferation, and oxidative processes, regardless of del(11q). Accordingly, BCR ligation with anti-IgM revealed a significant higher proliferation of subset #1 versus unmutated non-subset #1 CLL, both at baseline and after 24-48 hr stimulation. Subset #1 CLL represent a paradigmatic example of the direct link between BCR structure, function, and patients prognosis.

Original languageEnglish
Pages (from-to)74-82
Number of pages9
JournalAmerican Journal of Hematology
Volume89
Issue number1
DOIs
Publication statusPublished - Jan 2014

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