AI Article Synopsis

  • MicroRNAs are often improperly expressed in cancers, but their specific role in T-cell lymphoma, particularly Sézary Syndrome (SzS), was previously unclear.
  • In a study of T cells from 21 SzS patients, a unique microRNA expression profile was identified, with most miRNAs (104 of 114) being down-regulated, correlating with known genetic abnormalities.
  • Key findings included that miR-223 could effectively differentiate SzS patients from healthy controls and other conditions, and that the down-regulation of miR-342 contributes to SzS pathogenesis by inhibiting apoptosis, with additional insights on the regulation of miR-17-92 cluster in promoting cell apoptosis and limiting growth.

Article Abstract

MicroRNAs are commonly aberrantly expressed in many cancers. Very little is known of their role in T-cell lymphoma, however. We therefore elucidated the complete miRNome of purified T cells from 21 patients diagnosed with Sézary Syndrome (SzS), a rare aggressive primary cutaneous T-cell (CD4(+)) lymphoma. Unsupervised cluster analysis of microarray data revealed that the microRNA expression profile was distinct from CD4(+) T-cell controls and B-cell lymphomas. The majority (104 of 114) of SzS-associated microRNAs (P < .05) were down-regulated and their expression pattern was largely consistent with previously reported genomic copy number abnormalities and were found to be highly enriched (P < .001) for aberrantly expressed target genes. Levels of miR-223 distinguished SzS samples (n = 32) from healthy controls (n = 19) and patients with mycosis fungoides (n = 11) in more than 90% of samples. Furthermore, we demonstrate that the down-regulation of intronically encoded miR-342 plays a role in the pathogenesis of SzS by inhibiting apoptosis, and describe a novel mechanism of regulation for this microRNA via binding of miR-199a* to its host gene. We also provide the first in vivo evidence for down-regulation of the miR-17-92 cluster in malignancy and demonstrate that ectopic miR-17-5p expression increases apoptosis and decreases cell proliferation in SzS cells.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2938132PMC
http://dx.doi.org/10.1182/blood-2009-12-256719DOI Listing

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