Whang-Peng J, Knutsen T, Jaffe E S, Steinberg S M, Raffeld M, Zhao W P, Duffey P, Condron K, Yano T, Longo D L
Medicine Branch, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892.
Blood. 1995 Jan 1;85(1):203-16.
Few reports correlating specific cytogenetic abnormalities with distinct subtypes of lymphoma have performed serial studies at diagnosis and at tumor recurrence or progression. In our file of 325 cytogenetically analyzed non-Hodgkin's lymphoma (NHL) patients studied over the past decade, 43 had serial biopsies, 39 of whom had at least two successful preparations; of the 43, nine had one and 32 had two or more cytogenetically abnormal specimens. In this study, we correlated cytogenetic, histopathologic, molecular, and clinical parameters. Patients with low-grade lymphomas were as likely as patients with intermediate- or high-grade lymphomas to acquire new chromosomal abnormalities with time (16 of 23 patients as compared with 7 of 16; P2 = .11, chi 2 test). In four patients, originally diagnosed indolent disease progressed to aggressive disease; all had t(14;18), all gained additional chromosomal abnormalities with disease progression, and three of the four expressed abnormalities associated with disease progression and/or short survival: der(18), +7, and/or +12. Cytogenetic results from early disease were compared with those obtained later in disease: in the t(14;18) group, the most common abnormalities were +7 (eight patients) and der(18) (five patients), both seen later in disease. The most common abnormalities in patients without t(14;18) were 6q deletions; they were seen in both early and late disease and were associated with significantly shorter survivals (P2 = .0014) compared with all patients without 6q deletions. Secondary chromosomal abnormalities, observed after at least one previous abnormal study, were seen in 19 of 22 t(14;18) patients and in 11 of 21 patients without t(14;18) and were associated with a poor survival (P2 = .13) compared with patients without any secondary chromosomal abnormalities. Chromosome 1 abnormalities were seen in almost half of the patients and were observed in initial specimens and early in disease as well as late in disease and as secondary abnormalities; 1q involvement was more frequent than 1p (15 versus eight patients) and was significantly associated with poor survival only in patients with intermediate-/high-grade disease; the most common breakpoints were 1q21-q22 (nine patients) and 1p36 (six patients). Breakpoints at 2q21 and 3q27-q29 were limited to patients with t(14;18) and were almost exclusively secondary in nature. Molecular studies in 24 of our patients showed discrepancies with the cytogenetic results in only three patients: two had t(14;18) but no molecular rearrangements while two patients had no visible t(14;18) but were positive for major breakpoint region (MBR) rearrangement. The presence of MBR or minor breakpoint cluster (MCR) rearrangement had no apparent effect on survival.(ABSTRACT TRUNCATED AT 400 WORDS)
很少有将特定细胞遗传学异常与淋巴瘤不同亚型相关联的报告在诊断时以及肿瘤复发或进展时进行系列研究。在我们过去十年间进行细胞遗传学分析的325例非霍奇金淋巴瘤(NHL)患者档案中,43例进行了系列活检,其中39例至少有两次成功的标本制备;在这43例中,9例有一份标本,32例有两份或更多细胞遗传学异常标本。在本研究中,我们将细胞遗传学、组织病理学、分子学和临床参数进行了关联分析。低度淋巴瘤患者与中度或高度淋巴瘤患者一样,随着时间推移有获得新的染色体异常的可能(23例患者中有16例,而16例患者中有7例;P2 = 0.11,卡方检验)。4例最初诊断为惰性疾病的患者进展为侵袭性疾病;所有患者均有t(14;18),随着疾病进展均获得了额外的染色体异常,4例中有3例表现出与疾病进展和/或生存期短相关的异常:der(18)、+7和/或+12。将疾病早期的细胞遗传学结果与疾病后期获得的结果进行比较:在t(14;18)组中,最常见的异常是+7(8例患者)和der(18)(5例患者),均在疾病后期出现。无t(14;18)患者中最常见的异常是6q缺失;在疾病早期和晚期均可见,与所有无6q缺失的患者相比,生存期显著缩短(P2 = 0.0014)。在至少一次先前异常研究后观察到的继发性染色体异常,在22例t(14;18)患者中有19例出现,在21例无t(14;18)患者中有11例出现,与无任何继发性染色体异常的患者相比,生存期较差(P2 = 0.13)。几乎一半的患者出现1号染色体异常,在初始标本、疾病早期以及疾病晚期和作为继发性异常时均有观察到;1q受累比1p更常见(15例对8例患者),仅在中度/高度疾病患者中与生存期差显著相关;最常见的断点是1q21 - q22(9例患者)和1p36(6例患者)。2q21和3q27 - q29的断点仅限于t(14;18)患者,几乎完全是继发性的。对我们24例患者的分子学研究显示,仅3例患者的分子学结果与细胞遗传学结果存在差异:2例有t(14;18)但无分子重排,而2例患者无可见的t(14;18)但主要断点区域(MBR)重排呈阳性。MBR或微小断点簇(MCR)重排的存在对生存期无明显影响。(摘要截短至400字)
