"Subgroups of patients with chronic lymphocytic leukemia (CLL) have distinct expression profiles of Toll-like receptor (TLR) pathway-associated genes. To test the hypothesis that signaling through innate immunity receptors may influence the behavior of the malignant clone, we investigated the functional response triggered by the stimulaton of Toll-like receptors (TLRs) and NOD2 in 67 CLL cases assigned to different subgroups on the basis of IGHV gene usage, IGHV gene mutational status or B-cell receptor (BcR) stereotypy. Differences in the induction of co-stimulatory molecules and\/or apoptosis were observed in mutated vs. unmutated CLL. Different responses were also identified in subsets with stereotyped BcRs, underscoring the idea that "subset-biased" innate immunity responses may occur independently of mutational status. Additionally, differential modulation of kinase activities was induced by TLR stimulation of different CLL subgroups, revealing a TLR7-tolerant state for cases belonging to stereotyped subset #4. The distinct patterns of TLR\/NOD2 functional activity in cells from CLL subgroups defined by the molecular features of the clonotypic BcRs might prove relevant for elucidating the immune mechanisms underlying CLL natural history and for defining subgroups of patients who might benefit from treatment with specific TLR ligands."
Distinct Innate Immunity Pathways to Activation and Tolerance in Subgroups of Chronic Lymphocytic Leukemia with Distinct Immunoglobulin Receptors.
GHIA , PAOLO PROSPERO;CALIGARIS CAPPIO , FEDERICO;
2012-01-01
Abstract
"Subgroups of patients with chronic lymphocytic leukemia (CLL) have distinct expression profiles of Toll-like receptor (TLR) pathway-associated genes. To test the hypothesis that signaling through innate immunity receptors may influence the behavior of the malignant clone, we investigated the functional response triggered by the stimulaton of Toll-like receptors (TLRs) and NOD2 in 67 CLL cases assigned to different subgroups on the basis of IGHV gene usage, IGHV gene mutational status or B-cell receptor (BcR) stereotypy. Differences in the induction of co-stimulatory molecules and\/or apoptosis were observed in mutated vs. unmutated CLL. Different responses were also identified in subsets with stereotyped BcRs, underscoring the idea that "subset-biased" innate immunity responses may occur independently of mutational status. Additionally, differential modulation of kinase activities was induced by TLR stimulation of different CLL subgroups, revealing a TLR7-tolerant state for cases belonging to stereotyped subset #4. The distinct patterns of TLR\/NOD2 functional activity in cells from CLL subgroups defined by the molecular features of the clonotypic BcRs might prove relevant for elucidating the immune mechanisms underlying CLL natural history and for defining subgroups of patients who might benefit from treatment with specific TLR ligands."I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.