BACKGROUND: Prognostic index for survival estimation by clinical-demographic variables were previously proposed in chronic lymphocytic leukemia (CLL) patients. Our objective was to test in a large retrospective cohort of CLL patients the prognostic power of biological variables in a comprehensive model including clinical and demographic parameters. A new prognostic index was proposed.METHODS: Overall survival and time to treatment in 620 untreated CLL patients were analyzed retrospectively to evaluate the independent predictive power of mutational status of immunoglobulin heavy chain variable gene segments (IGHV), high-risk chromosomal aberration such as 17p or 11q deletions, CD38 and ZAP-70 expression, age, gender, Binet stage, beta2-microglobulin levels, absolute lymphocyte count and number of lymph node regions.RESULTS: IGHV mutational status and 17p deletion, but not CD38 and ZAP-70 expression, were independent prognostic biological variables in a multivariate model for overall survival, which included demographic (age and gender) and clinical parameters (Binet staging, beta2-microglobulin levels). Analysis of time to treatment in Binet A patients below 70 years of age showed that IGHV was the most important predictor. A novel 6-variable clinical-biological prognostic index was developed and internally validated, which assigned 3 points for Binet C stage, 2 points/each for Binet B stage and for age > 65 years, 1 point/each for male gender, high beta2-microglobulin levels, presence of an unmutated IGHV gene status or 17p deletion. Patients were classified at low-risk (score = 0-1; 21%), intermediate-risk (score 2-5; 63% of cases), high-risk (score 6-9; 16% of cases). Projected 5-year overall survival was 98%, 90% and 58% in low-, intermediate- and high-risk groups, respectively. A nomogram for individual patient survival estimation was also proposed.CONCLUSIONS: Data indicate that IGHV mutational status and 17p deletion may be integrated with clinical-demographic variables in new prognostic tools to estimate overall survival.
IGHV gene mutational status and 17p deletion are independent molecular predictors in a comprehensive clinical-biological prognostic model for overall survival prediction in chronic lymphocytic leukemia / Bulian, P; Rossi, D; Forconi, F; Del Poeta, G; Bertoni, F; Zucca, E; Montillo, M; Pozzato, G; D'Arena, G; Efremov, D; Marasca, Roberto; Lauria, F; Gaidano, G; Gattei, V; Laurenti, L.. - In: JOURNAL OF TRANSLATIONAL MEDICINE. - ISSN 1479-5876. - STAMPA. - 10:(2012), pp. 10-18. [10.1186/1479-5876-10-18]
IGHV gene mutational status and 17p deletion are independent molecular predictors in a comprehensive clinical-biological prognostic model for overall survival prediction in chronic lymphocytic leukemia.
MARASCA, Roberto;
2012
Abstract
BACKGROUND: Prognostic index for survival estimation by clinical-demographic variables were previously proposed in chronic lymphocytic leukemia (CLL) patients. Our objective was to test in a large retrospective cohort of CLL patients the prognostic power of biological variables in a comprehensive model including clinical and demographic parameters. A new prognostic index was proposed.METHODS: Overall survival and time to treatment in 620 untreated CLL patients were analyzed retrospectively to evaluate the independent predictive power of mutational status of immunoglobulin heavy chain variable gene segments (IGHV), high-risk chromosomal aberration such as 17p or 11q deletions, CD38 and ZAP-70 expression, age, gender, Binet stage, beta2-microglobulin levels, absolute lymphocyte count and number of lymph node regions.RESULTS: IGHV mutational status and 17p deletion, but not CD38 and ZAP-70 expression, were independent prognostic biological variables in a multivariate model for overall survival, which included demographic (age and gender) and clinical parameters (Binet staging, beta2-microglobulin levels). Analysis of time to treatment in Binet A patients below 70 years of age showed that IGHV was the most important predictor. A novel 6-variable clinical-biological prognostic index was developed and internally validated, which assigned 3 points for Binet C stage, 2 points/each for Binet B stage and for age > 65 years, 1 point/each for male gender, high beta2-microglobulin levels, presence of an unmutated IGHV gene status or 17p deletion. Patients were classified at low-risk (score = 0-1; 21%), intermediate-risk (score 2-5; 63% of cases), high-risk (score 6-9; 16% of cases). Projected 5-year overall survival was 98%, 90% and 58% in low-, intermediate- and high-risk groups, respectively. A nomogram for individual patient survival estimation was also proposed.CONCLUSIONS: Data indicate that IGHV mutational status and 17p deletion may be integrated with clinical-demographic variables in new prognostic tools to estimate overall survival.
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