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B细胞生长因子诱导毛细胞淋巴细胞增殖及Ⅰ型干扰素在体外的抑制作用。

B cell growth factor-induced proliferation of hairy cell lymphocytes and inhibition by type I interferon in vitro.

作者信息

Paganelli K A, Evans S S, Han T, Ozer H

出版信息

Blood. 1986 Apr;67(4):937-42.

PMID:2937473
Abstract

Malignant B cells from hairy cell leukemia (HCL) patients are unable to proliferate when stimulated with standard B cell mitogens. Using chromatographically purified B cell growth factor (BCGF), HCL can be stimulated to proliferate as assessed by incorporation of tritiated thymidine [3HTdR] into DNA. Proliferation was found to be time dependent, with no detectable 3H-TdR incorporation in up to three days of culture, and significant stimulation evident at days 6 and 10. The presence of 10% BCGF in culture was an absolute requirement for HCL proliferation; however, this BCGF-induced DNA synthesis could be further augmented by the addition of anti-immunoglobulin heavy chain antibodies. BCGF-induced proliferation was abrogated in six of six patients by addition of 1,000 U/mL of recombinant alpha 2-interferon (IFN) at day 0, although 1,000 U/mL of recombinant gamma-IFN had no inhibitory effect in five of six patients studied. Specific cellular receptors for type I IFN were demonstrated in HCL by inhibition of binding of 125I-alpha 2-IFN by a 40-fold excess of unlabeled alpha 2 or beta IFN with no inhibition by unlabeled gamma-IFN. These data demonstrate that malignant HCL lymphoblasts express specific type I IFN receptors and that type I, but not type II IFN, can inhibit growth factor-induced DNA synthesis by hairy cells in vitro. They further suggest a direct antiproliferative mechanism of action for IFN in HCL and predict equivalent clinical activity by either alpha or beta, but not gamma IFN in this malignancy.

摘要

毛细胞白血病(HCL)患者的恶性B细胞在受到标准B细胞有丝分裂原刺激时无法增殖。使用经色谱纯化的B细胞生长因子(BCGF),通过将氚化胸腺嘧啶核苷[3HTdR]掺入DNA来评估,可刺激HCL增殖。发现增殖具有时间依赖性,在培养长达三天时未检测到3H-TdR掺入,而在第6天和第10天有明显的刺激作用。培养物中存在10%的BCGF是HCL增殖的绝对必要条件;然而,添加抗免疫球蛋白重链抗体可进一步增强这种BCGF诱导的DNA合成。在第0天添加1000 U/mL的重组α2干扰素(IFN)可消除6例患者中6例的BCGF诱导的增殖,尽管在研究的6例患者中有5例,1000 U/mL的重组γ-IFN没有抑制作用。通过用40倍过量的未标记α2或β干扰素抑制125I-α2-IFN的结合,而未标记的γ-IFN无抑制作用,证明HCL中存在I型干扰素的特异性细胞受体。这些数据表明,恶性HCL淋巴母细胞表达特异性I型干扰素受体,并且I型而非II型干扰素可在体外抑制生长因子诱导的毛细胞DNA合成。它们进一步提示干扰素在HCL中的直接抗增殖作用机制,并预测α或β干扰素而非γ干扰素在这种恶性肿瘤中具有等效的临床活性。

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