| Literature DB >> 27995457 |
Taku Tsukamoto1, Miki Kiyota1,2, Eri Kawata3, Nobuhiko Uoshima3, Shotaro Tatekawa1, Yoshiaki Chinen1, Hisao Nagoshi1, Shinsuke Mizutani1, Yuji Shimura1, Mio Yamamoto-Sugitani1, Tsutomu Kobayashi1, Shigeo Horiike1, Satoru Yasukawa4, Akio Yanagisawa4, Masafumi Taniwaki1, Junya Kuroda5.
Abstract
Disease-specific cytogenetic abnormalities involving BCL2 gene rearrangement frequently co-exist with other cytogenetic abnormalities, contributing to disease progression in follicular lymphoma (FL). In the present study, we retrospectively investigated the prognostic impact of BCL2-unrelated cytogenetic abnormalities in FL. Of 139 consecutively diagnosed patients with FL at two independent institutes, metaphase spreads of tumor cells were obtained for use in G-banding analysis in 77 patients. The recurrent additional cytogenetic abnormalities included chromosome gains +5 (n = 8), +7 (n = 16), +12 (n = 10), and +X (n = 12), and losses -8 (n = 7), -13 (n = 12) -15 (n = 7), and 6q- (n = 7). While -15 was associated with shorter progression-free survival (PFS) in all 77 analyzed patients with evaluable G-banding results (p = 0.04), this negative impact was not evident in 42 patients treated using an R-CHOP-like regimen as first-line treatment. By contrast, 6q- was predictive for shorter PFS in patients who were initially treated with R-CHOP-like regimens without maintenance therapy (p < 0.01), while this negative impact was not evident in all 77 patients with evaluable G-banding results. These results suggest the presence of a molecular region in chromosome 6q that is responsible for the shorter PFS following R-CHOP-like chemotherapy.Entities:
Keywords: 6q−; Cytogenetics; Follicular lymphoma; Karyotype
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Year: 2016 PMID: 27995457 DOI: 10.1007/s12185-016-2166-0
Source DB: PubMed Journal: Int J Hematol ISSN: 0925-5710 Impact factor: 2.490