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The absolute percent deviation of IGHV mutation rather than a 98% cut-off predicts survival of chronic lymphocytic leukaemia patients treated with fludarabine, cyclophosphamide and rituximab

Authors :
Jain, P
Nogueras Gonzalez, GM
Kanagal-Shamanna, R
Rozovski, U
Sarwari, N
Tam, C
Wierda, WG
Thompson, PA
Jain, N
Luthra, R
Quesada, A
Sanchez-Petitto, G
Ferrajoli, A
Burger, J
Kantarjian, H
Cortes, J
O'Brien, S
Keating, MJ
Estrov, Z
Jain, P
Nogueras Gonzalez, GM
Kanagal-Shamanna, R
Rozovski, U
Sarwari, N
Tam, C
Wierda, WG
Thompson, PA
Jain, N
Luthra, R
Quesada, A
Sanchez-Petitto, G
Ferrajoli, A
Burger, J
Kantarjian, H
Cortes, J
O'Brien, S
Keating, MJ
Estrov, Z
Publication Year :
2018

Abstract

The degree of somatic hypermutation, determined as percent deviation of immunoglobulin heavy chain gene variable region sequence from the germline (IGHV%), is an important prognostic factor in chronic lymphocytic leukaemia (CLL). Currently, a cut-off of 2% deviation or 98% sequence identity to germline in IGHV sequence is routinely used to dichotomize CLL patients into mutated and unmutated groups. Because dissimilar IGHV% cut-offs of 1-5% were identified in different studies, we wondered whether no cut-off should be applied and IGHV% treated as a continuous variable. We analysed the significance of IGHV% in 203 CLL patients enrolled on the original frontline fludarabine, cyclophosphamide and rituximab (FCR) trial with a median of 10 years follow-up. Using the Cox Proportional Hazard model, IGHV% was identified as a continuous variable that is significantly associated with progression-free (PFS) and overall survival (OS) (P < 0·001). Furthermore, we validated this finding in 323 patients treated with FCR off-protocol and in the total cohort (n = 535). Multivariate analysis revealed a continuous trend. Higher IGHV% levels were incrementally associated with favorable PFS and OS in both FCR-treated cohorts (P < 0·001, both cohorts). Taken together, our data suggest that IGHV% is a continuous variable in CLL patients treated with FCR.

Details

Database :
OAIster
Publication Type :
Electronic Resource
Accession number :
edsoai.on1315677568
Document Type :
Electronic Resource