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成人急性淋巴细胞白血病中混合表型的表达模式

Expression pattern of hybrid phenotype in adult acute lymphoblastic leukemia.

作者信息

Nakase K, Kita K, Miwa H, Nishii K, Shiku H, Nasu K, Dohy H, Kyo T, Kamada N, Tsutani H

机构信息

Department of Internal Medicine, Saiseikai Matsusaka Hospital, Matsusaka, Japan.

出版信息

Cancer Detect Prev. 2001;25(4):394-405.

Abstract

We examined the expression of hybrid phenotype in 236 adults with acute lymphoblastic leukemia (ALL; 188 B-lineage ALL and 48 T-lineage ALL). In B-lineage ALL, myeloid antigen (mAg) CD15 was concentrated in CD10-CD20- cases (49%); CD13 (42%); and CD33 (43%) in CD10+CD20- cases. This trend had no correlation with the presence of Ph1 or t(4;11) chromosomal abnormality. T-cell antigen CD2, CD4, and CD7 was seen in four, four, and two cases, respectively, and CD4+ and CD7+ cases commonly expressed CD13 and/or CD33 (CD13/CD33). In T-lineage ALL, expression of mAg, CD11b (47%), CD13 (38%), CD15 (28%), and CD33 (51%) was restricted to CD3- cases. B-cell antigen CD19 was found in two cases with CD7 solely as T-cell antigen, and these cases possessed CD13/CD33. CD21 was detected in three cases with CD3. In whole ALL, CD13/CD33 was associated closely with the presence of stem-cell antigen CD34, and in T-lineage ALL, CD13/CD33 had a significant correlation with additional stem-cell features, such as HLA-DR, multidrug resistance 1 (MDR1) and c-kit gene expression. Our results suggest that immature ALL cells frequently express B+M+, T+M+, and occasionally B+T+M+ phenotype; that B+T+M- phenotype is extremely rare; and that mAg expression in B-lineage ALL is complicated as compared to T-lineage ALL.

摘要

我们检测了236例成人急性淋巴细胞白血病(ALL;188例B系ALL和48例T系ALL)中混合表型的表达情况。在B系ALL中,髓系抗原(mAg)CD15在CD10-CD20-病例中表达集中(49%);CD13在CD10+CD20-病例中表达(42%);CD33在CD10+CD20-病例中表达(43%)。这种趋势与Ph1或t(4;11)染色体异常的存在无关。T细胞抗原CD2、CD4和CD7分别在4例、4例和2例中可见,且CD4+和CD7+病例通常表达CD13和/或CD33(CD13/CD33)。在T系ALL中,mAg CD11b(47%)、CD13(38%)、CD15(28%)和CD33(51%)的表达仅限于CD3-病例。B细胞抗原CD19在2例仅以CD7作为T细胞抗原的病例中被发现,且这些病例具有CD13/CD33。CD21在3例CD3阳性的病例中被检测到。在整个ALL中,CD13/CD33与干细胞抗原CD34的存在密切相关,而在T系ALL中,CD13/CD33与其他干细胞特征,如HLA-DR、多药耐药1(MDR1)和c-kit基因表达显著相关。我们的结果表明,不成熟的ALL细胞经常表达B+M+、T+M+,偶尔表达B+T+M+表型;B+T+M-表型极其罕见;并且与T系ALL相比,B系ALL中mAg的表达更为复杂。

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