Glinsky G V, Price J E, Glinsky V V, Mossine V V, Kiriakova G, Metcalf J B
Cancer Research Center, Department of Biochemistry, University of Missouri, Columbia 65201, USA.
Cancer Res. 1996 Dec 1;56(23):5319-24.
We have examined the effect of synthetic low molecular weight glycoamine analogues on the metastasis of MDA-MB-435 human breast carcinoma xenografts growing in the mammary fat pads of nude mice. Initial in vitro screening of a panel of synthetic glycoamines was performed using a clonogenic growth assay in 0.9% agarose. Eight of nine compounds manifested a significant dose-dependent inhibition of colony formation by MDA-MB-435 cells in 0.9% agarose. The relative activity ranks of the compounds, based on ID50S independently determined for each synthetic glycoamine analogue, identified N-(1-deoxy-D-lactulos-1-yl)-L-leucine (Lac-L-Leu), N-(1-deoxy-D-fructos-1-yl)-D-leucine (Fru-D-Leu), N-(1-deoxy-D-fructos-1-yl)-L-phenylalanine, and N-(1-deoxy-D-fructos-1-yl)-L-leucine as the most effective inhibitors of colony formation. Two separate experimental treatment protocols were used to examine the effect of selected synthetic glycoamines on human breast cancer growth and metastasis in athymic nude mice. Group A mice were treated intraperitoneally daily from day 2 after injection of the breast cancer cells until the end of the experiment (17 weeks). In group B, the mice were untreated until the mean tumor diameter was 10 mm, at which time daily i.p. treatment began. After 7 days, the primary tumors were resected, and the mice were treated for an additional 4 weeks (a total of 5 weeks of treatment). The synthetic glycoamines did not have significant antitumor effects, and there was no difference in the tumor incidence or tumor growth rates in mice treated continuously with synthetic glycoamines or PBS. The significant antimetastatic activity of synthetic glycoamines was detected in both experimental treatment protocols. In mice continuously treated with synthetic glycoamines according to protocol A, the incidence of metastasis was decreased 4.6-fold (P = 0.014) and 2.7-fold (P = 0.031) in mice treated with Fru-D-Leu and Lac-L-Leu, respectively. In mice in protocol B, the incidence of pulmonary metastasis was decreased 1.9-fold (P = 0.069) and 2.5-fold (P = 0.042) in mice treated with Fru-D-Leu and Lac-L-Leu, respectively. Correspondingly, the average number of spontaneous pulmonary metastases was reduced from 37 in control mice to 0.2 (P = 0.005) and 0.9 (P < 0.02) in mice treated according to the protocol A with Fru-D-Leu and Lac-L-Leu, respectively. Treatment of mice with N-(1-deoxy-D-fructos-1-yl)-L-leucine did not have significant antimetastatic effects, and no reduction in metastasis incidence or number was noted in mice treated with this synthetic glycoamine analogue. The treated animals had no apparent toxicity from chronic daily injection (up to 17 weeks of treatment) of synthetic glycoamines, and no obvious pathology was noted in the histological slides of the livers, kidneys, or spleens of the treated mice. Therefore, we have identified two synthetic glycoamines (Fru-D-Leu and Lac-L-Leu) that were the effective inhibitors of spontaneous human breast cancer metastasis in nude mice. Potential mechanisms for antimetastatic activity of synthetic glycoamines may include the inhibition of beta-galectin-mediated homotypic cancer cell aggregation and induction of apoptosis in target cells.
我们研究了合成的低分子量糖胺类似物对在裸鼠乳腺脂肪垫中生长的人MDA-MB-435乳腺癌异种移植物转移的影响。使用在0.9%琼脂糖中的克隆形成生长试验对一组合成糖胺进行了初步体外筛选。九种化合物中的八种在0.9%琼脂糖中对MDA-MB-435细胞的集落形成表现出显著的剂量依赖性抑制作用。根据为每种合成糖胺类似物独立测定的ID50确定的化合物相对活性等级,确定N-(1-脱氧-D-乳酮糖-1-基)-L-亮氨酸(Lac-L-Leu)、N-(1-脱氧-D-果糖-1-基)-D-亮氨酸(Fru-D-Leu)、N-(1-脱氧-D-果糖-1-基)-L-苯丙氨酸和N-(1-脱氧-D-果糖-1-基)-L-亮氨酸是最有效的集落形成抑制剂。使用两种不同的实验治疗方案来研究选定的合成糖胺对无胸腺裸鼠人乳腺癌生长和转移的影响。A组小鼠在注射乳腺癌细胞后第2天开始每天腹腔注射,直至实验结束(17周)。在B组中,小鼠在平均肿瘤直径达到10 mm之前不进行治疗,此时开始每天腹腔注射治疗。7天后,切除原发性肿瘤,小鼠再接受4周治疗(总共治疗5周)。合成糖胺没有显著的抗肿瘤作用,连续用合成糖胺或PBS治疗的小鼠在肿瘤发生率或肿瘤生长速率方面没有差异。在两种实验治疗方案中均检测到合成糖胺的显著抗转移活性。在按照方案A连续用合成糖胺治疗的小鼠中,用Fru-D-Leu和Lac-L-Leu治疗的小鼠转移发生率分别降低了4.6倍(P = 0.014)和2.7倍(P = 0.031)。在方案B的小鼠中,用Fru-D-Leu和Lac-L-Leu治疗的小鼠肺转移发生率分别降低了1.9倍(P = 0.069)和2.5倍(P = 0.042)。相应地,自发肺转移的平均数量从对照小鼠的37个分别减少到按照方案A用Fru-D-Leu和Lac-L-Leu治疗小鼠的0.2个(P = 0.005)和0.9个(P < 0.02)。用N-(1-脱氧-D-果糖-1-基)-L-亮氨酸治疗小鼠没有显著的抗转移作用,在用这种合成糖胺类似物治疗的小鼠中未观察到转移发生率或数量的降低。经治疗的动物在每天慢性注射(长达17周治疗)合成糖胺后没有明显毒性,在经治疗小鼠的肝脏、肾脏或脾脏组织切片中未观察到明显病变。因此,我们确定了两种合成糖胺(Fru-D-Leu和Lac-L-Leu),它们是裸鼠中自发人乳腺癌转移的有效抑制剂。合成糖胺抗转移活性的潜在机制可能包括抑制β-半乳糖凝集素介导的同型癌细胞聚集和诱导靶细胞凋亡。
