Cooper Andrew C, Karp Russell M, Clark Edward J, Taghizadeh Nazbeh R, Hoyt Jennifer G, Labenski Matthew T, Murray Michael J, Hannig Gerhard, Westlin William F, Thompson Charles D
Department of Cell Biology, Repligen, Waltham, Massachusetts, USA.
Clin Cancer Res. 2006 Apr 15;12(8):2583-90. doi: 10.1158/1078-0432.CCR-05-0871.
Fumagillin and related compounds have potent antiproliferative activity through inhibition of methionine aminopeptidase-2 (MetAP-2). It has recently been reported that MetAP-2 is highly expressed in germinal center B cells and germinal center-derived non-Hodgkin's lymphomas (NHL), suggesting an important role for MetAP-2 in proliferating B cells. Therefore, we determined the importance of MetAP-2 in normal and transformed germinal center B cells by evaluating the effects of MetAP-2 inhibition on the form and function of germinal centers and germinal center-derived NHL cells.
To examine the activity of PPI-2458 on germinal center morphology, spleen sections from cynomolgus monkeys treated with oral PPI-2458 were analyzed. Antiproliferative activity of PPI-2458 was assessed on germinal center-derived NHL lines in culture. A MetAP-2 pharmacodynamic assay was used to determine cellular MetAP-2 inhibition following PPI-2458 treatment. Finally, inhibition of MetAP-2 and proliferation by PPI-2458 was examined in the human SR NHL line in culture and in implanted xenografts.
Oral PPI-2458 caused a reduction in germinal center size and number in lymphoid tissues from treated animals. PPI-2458 potently inhibited growth (GI(50) = 0.2-1.9 nmol/L) of several NHL lines in a manner that correlated with MetAP-2 inhibition. Moreover, orally administered PPI-2458 significantly inhibited SR tumor growth, which correlated with inhibition of tumor MetAP-2 (>85% at 100 mg/kg) in mice.
These results show the potent antiproliferative activity of PPI-2458 on NHL lines in vitro and oral antitumor activity in vivo and suggest the therapeutic potential of PPI-2458 as a novel agent for treatment of NHL should be evaluated in the clinical setting.
烟曲霉素及相关化合物通过抑制甲硫氨酸氨基肽酶-2(MetAP-2)具有强大的抗增殖活性。最近有报道称,MetAP-2在生发中心B细胞和生发中心来源的非霍奇金淋巴瘤(NHL)中高表达,提示MetAP-2在增殖性B细胞中起重要作用。因此,我们通过评估MetAP-2抑制对生发中心及生发中心来源的NHL细胞的形态和功能的影响,确定MetAP-2在正常和转化的生发中心B细胞中的重要性。
为检测PPI-2458对生发中心形态的活性,分析了经口服PPI-2458处理的食蟹猴的脾脏切片。在培养的生发中心来源的NHL细胞系上评估PPI-2458的抗增殖活性。使用MetAP-2药效学测定法确定PPI-2458处理后细胞内MetAP-2的抑制情况。最后,在培养的人SR NHL细胞系和植入的异种移植物中检测PPI-2458对MetAP-2和增殖的抑制作用。
口服PPI-2458导致处理动物淋巴组织中生发中心大小和数量减少。PPI-2458以与MetAP-2抑制相关的方式强烈抑制几种NHL细胞系的生长(GI(50)=0.2-1.9 nmol/L)。此外,口服PPI-2458显著抑制SR肿瘤生长,这与小鼠肿瘤MetAP-2的抑制相关(100 mg/kg时>85%)。
这些结果显示了PPI-2458在体外对NHL细胞系具有强大的抗增殖活性以及在体内具有口服抗肿瘤活性,并提示PPI-2458作为治疗NHL的新型药物的治疗潜力应在临床环境中进行评估。
