CN100464783C - 一种含抗肿瘤抗生素的抗癌药物组合物 - Google Patents
一种含抗肿瘤抗生素的抗癌药物组合物 Download PDFInfo
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- CN100464783C CN100464783C CNB2004100360978A CN200410036097A CN100464783C CN 100464783 C CN100464783 C CN 100464783C CN B2004100360978 A CNB2004100360978 A CN B2004100360978A CN 200410036097 A CN200410036097 A CN 200410036097A CN 100464783 C CN100464783 C CN 100464783C
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Abstract
一种抗癌药物组合物,属于药物技术领域。由药用辅料以及包于其中的抗肿瘤药物组成。其中抗肿瘤药物为抗肿瘤抗生素。药用辅料主要为生物可容性可降解吸收的高分子多聚物,在其降解吸收的过程中能将抗癌药物缓慢释放于肿瘤局部,因此在明显降低其全身毒性反应的同时还可于肿瘤局部维持有效药物浓度。该抗癌药物组合物肿瘤局部放置。该组合物不仅能够降低药物的全身毒性反应,同时还能选择性地提高肿瘤局部的药物浓度,增强化疗药物及放射治疗等非手术疗法的治疗效果。
Description
(一)技术领域
本发明涉及一种抗癌药物组合物,属于药物技术领域。
(二)背景技术
癌症的治疗主要包括手术、放疗及化疗等方法。在所用的各种化疗药物中,抗肿瘤抗生素的作用效果较为明显,已广泛应用于多种恶性肿瘤。然而,肿瘤间质中的血管、结缔组织、基质蛋白、纤微蛋白及胶原蛋白等不仅为肿瘤细胞的生长提供了支架及必不可少的营养物质,还影响了化疗药物在肿瘤周围及肿瘤组织内的渗透和扩散(参见尼提等“细胞外间质的状况对实体肿瘤内药物运转的影响”《癌症研究》60期2497-503页(2000年)(Netti PA,Cancer Res.2000,60(9):2497-503)。由于实体肿瘤过度膨胀性增生,其间质压力、组织弹性压力、流体压力及间质的粘稠度均较其周围正常组织为高,因此,常规化疗,难于肿瘤局部形成有效药物浓度(参见孔庆忠等“瘤内放置顺铂加系统卡莫司汀治疗大鼠脑肿瘤”《外科肿瘤杂志》69期76-82页(1998年)(Kong Q et al.,J Surg Oncol.1998 Oct;69(2):76-82),单纯提高给药剂量又受到全身反应的限制。因此,本发明的一个具体的主题是抗癌药物组合物,以能够提高肿瘤局部的药物浓度以及肿瘤细胞对药物的敏感程度为要旨。
(三)发明内容
本发明针对现有技术的不足,提供一种抗癌药物组合物。
本发明抗癌药物组合物,包括抗癌有效成分和药用辅料。其中抗癌有效成分为抗肿瘤抗生素,抗肿瘤抗生素选自7-O-甲基诺加-4’-表阿霉素(7-o-methylnogallol-4’-epiadriamycin,mDox)、克拉霉素(Clarithromycin)、阿克拉霉素(Aclacinomycin A、aclarubicin、ACLA、阿柔比星)、阿克拉霉素-B、氨柔比星(Amrubicin)、4’-(辣根联苯氨甲氧基苯醯腆胺)[4′-(acridinylamino)methansulfon-m-anisidide,m-AMSA]、4-去甲氧道诺红菌素(4-demethoxydaunorubicin)、地托比星、表柔比星(Epirubicin)、依索比星(Esorubicin)、卡柔比星、伊达比星(idarubicin,IDA)、罗多比星、流柔比星(Leurubicin)、美多比星、奈莫柔比星(Nemorubicin)、多柔比星、吡柔比星(Pirarubicin)、奥柔比星(N-三氟毒素-14-戊酸盐、N-trifluoroacetyladriamycin-14-valerate,AD32,valrubicin)、2-[4-(7-氯-2-喹喔啉基氧苯氧基)-丙酸((2-[4-(7-chloro-2-quinoxalinyloxyphenoxy)-propionic acid,XK469)、佐柔比星(Zorubicin)、N-(2-氯乙烷)-N-亚硝基脲基柔红霉素(N-(2-Chloroethyl)-N-nitrosoureidodaunorubicin,AD312)、洛撒蒽醌、洛索蒽醌[Losoxantrone]、吡罗蒽醌[Piroxantrone]、替洛蒽醌[Teloxantrone]、癌霉素、派来霉素、硫酸派来霉素、抗生素1588、波外定、盐酸阿可达佐、阿可达佐、克大霉素、乙酰克大霉素(乙酰贵田霉素)、阿佐霉素(含氮霉素)、蛇形菌素(Diacetoxysciroenol)、三铁阿霉素、二乙氧醋酰阿霉素、环霉素、消癌菌素(carzinocidin)、嗜癌素(carzinophylin)、嗜癌霉素、瘤菌素、治癌菌素(carzinostatin,制癌菌素)、重氮霉素(diazamycine)、大菌素(macrocin)、大菌霉素(macrocinomycin)、丙氨菌素、丙氨肽霉素、阿乐盖、新丝菌素(neothricin,neothramycin)、大分子霉素(macromomycin或macromycin)、新塞那霉素、诺卡菌素(nocardin)、诺卡菌红素(nocardorubin)、诺卡型霉素(noformicin)、诺加霉素(诺加拉霉素,nogalamycin or nogaromycin)、丝裂红素(mitochromine ormitocromine)、多粘菌素E(Polymyxin E)、吡利霉素(Pirlimycin)、地红霉素(Dirithromycin)、安曲霉素、恶溶菌素、达佐霉素、橄榄霉素、链黑霉素、链黑霉素甲酯、链脲霉素、培洛霉素、嘌罗霉素、司帕霉素、他利霉素、羟硝氨糖环素、蒽霉素(氨茴霉素,安拉霉素)、甲基蒽霉素、艾菲地可宁、曲林菌素、(盐酸)卡米诺霉素、他利霉素、巨毛霉素、去甲柔毛霉素、氯脲霉素、色霉素A3、氯佐星(chlorozotocin)、去甲利福平、蒽环霉素-A、黑他七霉素、脱氧助间型霉素、嘌呤霉素、盐酸嘌呤霉素、雷查霉素、瑞必克霉素、桑霉素、抗癌霉素、西伯利亚霉素、他利霉素、米托佐罗、硒唑呋喃、斯潘格宁、盐酸锗螺胺、锗螺胺、螺妙斯定或抗癌锑等。
上述抗肿瘤抗生素可单选或多选。其中优选7-O-甲基诺加-4’-表阿霉素、阿柔比星、阿克拉霉素-B、氨柔比星、4’-(辣根联苯氨甲氧基苯醯腆胺)[m-AMSA]、4-去甲氧道诺红菌素、地托比星、表柔比星、依索比星、卡柔比星、伊达比星、罗多比星、流柔比星、美多比星、奈莫柔比星、多柔比星、吡柔比星、奥柔比星、2-[4-(7-氯-2-喹喔啉基氧苯氧基]-丙酸、佐柔比星(Zorubicin)、N-(2-氯乙烷)-N-亚硝基脲基柔红霉素(AD 312)、洛撒蒽醌、洛索蒽醌、吡罗蒽醌、替洛蒽醌、阿可达佐、二乙氧醋酰阿霉素或治癌菌素。
上述抗肿瘤抗生素在组合物中的重量百分比含量可从0.1%—80%,以1%—50%为佳,以2%—30%为最佳。
本发明抗癌药物组合物的优选抗癌有效成分如下,均为重量百分比:
(a)1%—50%7-O-甲基诺加-4’-表阿霉素、阿柔比星、阿克拉霉素-B、氨柔比星、4’-(辣根联苯氨甲氧基苯醯腆胺)、4-去甲氧道诺红菌素、地托比星、表柔比星、依索比星、卡柔比星、伊达比星、罗多比星、流柔比星、美多比星、奈莫柔比星、多柔比星、吡柔比星、奥柔比星、2-[4-(7-氯-2-喹喔啉基氧苯氧基]-丙酸、佐柔比星或N-(2-氯乙烷)-N-亚硝基脲基柔红霉素;
(b)1%—50%洛撒蒽醌、洛索蒽醌、吡罗蒽醌、替洛蒽醌、癌霉素、派来霉素、硫酸派来霉素、抗生素1588、波外定、盐酸阿可达佐、阿可达佐、克大霉素、乙酰克大霉素、阿佐霉素、蛇形菌素、三铁阿霉素、二乙氧醋酰阿霉素、环霉素、消癌菌素、嗜癌素、嗜癌霉素、瘤菌素、治癌菌素、重氮霉素、大菌素、大菌霉素、丙氨菌素或丙氨肽霉素;
(c)1%—50%阿乐盖、新丝菌素、大分子霉素、新塞那霉素、诺卡菌素、诺卡菌红素、诺卡型霉素、诺加霉素、丝裂红素、多粘菌素E、吡利霉素、地红霉素、安曲霉素、恶溶菌素、达佐霉素、橄榄霉素、链黑霉素、链黑霉素甲酯、链脲霉素、培洛霉素、嘌罗霉素、司帕霉素、他利霉素、羟硝氨糖环素、蒽霉素、甲基蒽霉素、艾菲地可宁或曲林菌素;
(d)1%—50%(盐酸)卡米诺霉素、他利霉素、巨毛霉素、去甲柔毛霉素、氯脲霉素、色霉素A3、氯佐星、去甲利福平、蒽环霉素-A、黑他七霉素、脱氧助间型霉素、嘌呤霉素、盐酸嘌呤霉素、雷查霉素、瑞必克霉素、桑霉素、抗癌霉素、西伯利亚霉素、他利霉素、米托佐罗、硒唑呋喃、斯潘格宁、盐酸锗螺胺、锗螺胺、螺妙斯定或抗癌锑等。
药用辅料包括下列之一:
(1)生物相容性高分子多聚物,包括生物可降解的或生物不可降解的多聚物及其混合物或共聚物,(2)水溶性低分子化合物,(3)用于实现针剂和缓释剂等药物剂型的合适的添加剂及赋型剂。
上述生物可降解的多聚物包括天然的和/或合成的多聚物。合成的多聚物如,但不限于,聚酐类、聚羟基酸、聚酯(polyesters)、聚酰胺(polyamides)、聚原酸酯(polyorthoesters)、聚磷腈(polyphosphazenes)、对羧苯基丙烷(p-CPP)、葵二酸(sebacic acid)等;天然的多聚物如,但不限于,蛋白质及多糖,包括透明质酸、胶原蛋白、明胶、白蛋白等。
上述聚酐类可选用,但不限于,芳香聚酐、脂肪族聚酐;其中芳香聚酐将解较慢,熔点高,有机溶剂中溶解度低,然而,芳香聚酐与脂肪族聚酐的共聚物却较为理想(美国专利4757128)。其代表物是聚苯丙生(对羧苯基丙烷(p-CPP)与葵二酸(SA)的共聚物),而对羧苯基丙烷为芳香聚酐,葵二酸则是一个芳香二酸与一个脂肪二酸的共聚物。可选用的其它芳香或脂肪族聚酐的共聚物在其它美国专利中已有详细描述,如US4857311;4888176;4789724。
上述聚羟基酸可选用,但不限于,聚乳酸(PLA)、聚乙醇酸(PGA)、聚乳酸(PLA)与聚乙醇酸的混合物、乙醇酸和羟基羧酸的共聚物(PLGA);当PLA和PLGA混合时,其含量重量百分比分别为0.1-99.9%和99.9-0.1%。聚乳酸的分子量可为,但不限于,5000—100,000,但以10,000—50000为优选,以10,000—20000为最优选;聚乙醇酸的分子量可为,但不限于,5000—100,000,但以10,000—50000为优选,以10,000—20000为最优选;以上聚羟基酸可单选或多选。当单选时,以聚乳酸(PLA)或羟基羧酸和乙醇酸的共聚物(PLGA)为优选,共聚物的分子量可为,但不限于,1000—100,000,但以10,000—50000为优选;以10,000—20000为最优选;当多选时,以高分子多聚物或不同高分子多聚物组成的复合多聚物或共聚物为优选,以含不同分子量聚乳酸或葵二酸的复合多聚物或共聚物为最优选,如,但不限于,分子量为5000到10000的聚乳酸与分子量为20000到50000的聚乳酸混合、分子量为10000到20000的聚乳酸与分子量为30000到80000的PLGA混合、分子量为5000到10000的聚乳酸与葵二酸混合、分子量为30000到80000的PLGA与葵二酸混合。
上述生物不可降解的多聚物包括,但不限于:有机硅聚合物、乙烯乙酸乙烯酯共聚物(Ethelene-vinyl acetate copolymer,EVAc)、聚丙烯腈(polyacrylonitriles),聚氨基甲酸酯(polyurethanes)及聚磷腈(polyphosphazenes)等。组合物可通过直接扩散的方式将有效成分释放出来。
为调节药物释放速度或改变本发明抗癌组合物的其它特性,可以改变聚合物的单体成分或分子量、添加或调节药用辅料的组成及配比,添加水溶性低分子化合物,如,但不限于,各种糖和盐等。其中糖可为,但不限于,木糖醇、低聚糖及甲壳素等,其中盐可为但不限于,钾盐和钠盐等。
本发明抗癌组合物所用的药用辅料可为上述药用辅料中的任何一种或多种物质,但以水溶性高分子聚合物为主选,在各种高分子聚合物中,以聚乳酸、葵二酸、含聚乳酸或葵二酸的高分子多聚物的混合物或共聚物为首选,混合物和共聚物可选自,但不限于,PLGA、乙醇酸和羟基羧酸的混合物、葵二酸与芳香聚酐或脂肪族聚酐的混合物或共聚物。乙醇酸和羟基羧酸的共混比例是10/90-90/10(重量),最好是25/75-75/25(重量)。共混的方法是任意的。乙醇酸和羟基羧酸共聚时的含量分别为重量百分比10-90%和90-10%。芳香聚酐的代表物是对羧苯基丙烷(p-CPP),对羧苯基丙烷(p-CPP)与葵二酸共聚时的含量分别为重量百分比10-60%和20-90%,共混重量比是10-40:50-90,最好是重量比15-30:65-85。
药用辅料在《药用辅料大全》(第123页,四川科学技术出版社1993年出版,罗明生和高天惠主编)中已有详细描述。另外,中国专利(申请号96115937.5;91109723.6;9710703.3;01803562.0)及美国发明专利(专利号5,651,986)也列举了某些药用辅料。包括充填剂、增溶剂、吸收促进剂、成膜剂、胶凝剂、制(或致)孔剂、赋型剂或阻止剂。以上药用辅料有的具有多重作用,因此有的同种物质被列为不同的类别。本发明抗实体肿瘤组合物可选用的支持物可为上述药用辅料中的任何一种或多种物质,并不完全根据其分类或定义来限制组合物的技术特征。
抗癌药物组合物的有效成分可均匀地包装于整个药用辅料中,也可包装于载体支持物中心或其表面;可通过直接扩散或经多聚物降解的方式或如此两种方式将有效成分释放。除此之外,抗癌药物组合物的有效成分也可均匀地包装于脂质体中,或以现有技术方法制成微球。
本发明的特点在于所用的药用辅料除高分子聚合物外,还含有上述任意一种或多种其它药用辅料。添加的药用辅料统称为添加剂。添加剂可根据其功能分为充填剂、致孔剂、赋型剂、分散剂、等渗剂、保存剂、阻止剂、增溶剂、吸收促进剂、成膜剂、胶凝剂等。
药用辅料还可为流质,如,但不限于芝麻油、混悬液、蒸馏水、生理冲液、以及半固态物质,如(但不限于)果冻、糊剂、软膏等,上述药用辅料适用于含或不含添加剂的组合物。
本发明抗癌药物组合物可制成多种剂型。如,但不限于,针剂、混悬液、软膏、胶囊及缓释剂等;呈各种形状,如,但不限于,颗粒样、片状、球形、块状、针状、棒状及膜状。在各种剂型中,以体内缓慢释放剂为主。上述剂型和形状适用于含或不含添加剂的组合物。
由于本发明抗癌药物组合物可使常规化疗、免疫治疗、高热治疗、光化学治疗、电疗、生物治疗、激素治疗、磁疗、超声治疗、放疗及基因治疗等方法的作用效果加强。因此在局部缓慢释放的同时可与上述非手术疗法合用,从而使其抗癌效果进一步加强。
当与上述非手术疗法合用时,本发明抗癌药物组合物可与非手术疗法同时应用,也可在非手术疗法实施前几天内应用,其目的在于尽可能增强肿瘤的敏感性。从而为根治各种人体及动物原发和转移实体肿瘤提供一种更有效的新的方法,具有非常高的临床应用价值及显著的经济和社会效益。
给药途径
本发明抗癌药物组合物可经各种途径应用,如静脉、动脉、皮下、肌肉、皮内、腔内、瘤内、瘤周等。给药途径取决于多种因素,如肿瘤所在部位、是否手术或转移、肿瘤体积大小、肿瘤类别、病人年龄、身体状况、生育状况及要求等。为于肿瘤所在部位获得有效药物浓度,可选择性地动脉灌注,腔内灌注(intracavitary),腹腔(intraperitoneal)或胸腔(intrapleural)及椎管内(intraspinal)给药,也可脏器内放置,如肠腔内、膀胱内、宫腔内、阴道内、胃内及食道内等。在多种途径中,以局部给药,如以选择性动脉、瘤内、瘤周注射为主,以瘤内、瘤周或瘤腔缓慢释放的形式为优选,如可选用多种缓释泵及缓释胶囊或体内缓释植入剂。
给药剂量
抗癌药物的用量取决于很多因素,如,但不限于,肿瘤体积、病人体重、给药方式、病情进展情况及治疗反应。有效剂量为0.01-80毫克/公斤体重,以1-50毫克/公斤体重为理想,以2-10毫克/公斤体重为最理想。抗癌药物在组合物中所占的比例因具体情况而定,可从0.1%—80%,以1%—50%为佳,以2%—30%为最佳。均为重量百分比。
本发明抗癌药物组合物可以用于制备治疗人、宠物及各种动物的各种癌、肉瘤或癌肉瘤等实体肿瘤的药物,包括起源于大脑、中枢神经系统、肾脏、肝、胆囊、头颈部、口腔、甲状腺、皮肤、黏膜、腺体、血管、骨组织、淋巴结、肺脏、食管、胃、乳腺、胰腺、眼睛、鼻咽部、子宫、卵巢、子宫内膜、子宫颈、前列腺、膀胱、结肠、直肠的原发或转移的癌或肉瘤或癌肉瘤。
该抗癌药物组合物中还可加入其它药用成分,如,但不限于,抗菌素、止疼药、抗凝药、止血药等。以上药用成分可单选或多选,可加入到含或不含添加剂的组合物,其含量因具体需要而定。
将上述有效成分包装于药用辅料中,然后局部应用。该组合物可经各种途径给药,以局部给药,如选择性动脉注射和直接瘤体内注射为佳,其中又以局部缓慢释放为最佳。当局部应用时,本发明抗癌药物组合物可直接置于原发或转移的实体肿瘤周围或瘤体内,也可直接置于原发或转移的实体肿瘤全部或部分切除后所形成的腔内。
本发明抗癌药物组合物主要成份以生物可容性物质为支持物,故不引起异物反应。支持物体内放置后可降解吸收,故不再手术取出。因在肿瘤局部释放所含药物,从而选择性地提高并延长局部药物浓度,同时可降低由常规途径给药所造成的全身毒性反应。
抗癌药物组合物可制成各种形状,其中有效成份的含量因不同需要而定。可从0.1%—80%,以1%—50%为佳,以2%—30%为最佳。均为重量百分比。该抗癌药物组合物可制成各种剂型,如,但不限于,针剂、混悬液、软膏、胶囊、及植入(缓释)剂等;呈各种形状,如,但不限于,颗粒样、片状、球形、块状、针状、棒状及膜样;可经各种途径给药,以动脉途径为佳,肿瘤体内直接放置为最佳。本发明的最佳剂型为生物可容性、可降解吸收的植入缓释剂,可因不同临床需要而制成各种形状。其主要成份的包装方法和步骤在美国专利中(US5651986)已有详细描述,包括若干种制备缓释制剂的方法:如,但不限于,(i)把载体支持物粉末与药物混合然后压制成植入剂,即所谓的混合法;(ii)把载体支持物熔化,与待包装的药物相混合,然后固体冷却,即所谓的熔融法;(iii)把载体支持物溶解于溶剂中,把待包装的药物溶解或分散于聚合物溶液中,然后蒸发溶剂,乾燥,即所谓的溶解法。其中溶解法可用以微球的制造,其方法是任意的,抗癌药物组合物也可包装于脂质体中。
本发明抗癌药物组合物制备技术的特点在于将抗肿瘤抗生素包装于药用辅料中,按照一定比例将有效成份和药用辅料溶解,待充份混匀之后乾燥。待乾燥后立即成形并消毒分装。
试验一、抗肿瘤抗生素的体外抑瘤作用。
所用的肿瘤细胞包括CNS-1、C6、胃腺上皮癌(SA)、骨肿瘤(BC)、乳腺癌(BA)、肺癌(LH)、甲状腺乳头状腺癌(PAT)、肝癌等。将以下抗肿瘤抗生素按10ug/ml浓度加到体外培养24小时的各种肿瘤细胞中,继续培养48小时后计数细胞总数。其肿瘤生长抑制效果见表1所示。
表1
| 瘤细胞 | Val | mDox | AD312 | ACLA | Piro | Am | Eso | mAMSA | IDA |
| CNS | 68% | 64% | 62% | 66% | 76% | 64% | 62% | 66% | 67% |
| C6 | 62% | 64% | 76% | 60% | 74% | 64% | 66% | 60% | 64% |
| SA | 60% | 60% | 68% | 56% | 72% | 60% | 66% | 66% | 72% |
| BC | 52% | 64% | 74% | 54% | 74% | 54% | 64% | 64% | 74% |
| BA | 50% | 62% | 68% | 62% | 62% | 52% | 66% | 62% | 72% |
| LH | 62% | 58% | 72% | 62% | 62% | 68% | 72% | 62% | 62% |
| PAT | 58% | 56% | 74% | 66% | 62% | 66% | 74% | 66% | 64% |
注解:Val:奥柔比星;mDox:7-O-甲基诺加-4’-表阿霉素;AD312:N-(2-氯乙烷)-N-亚硝基脲基柔红霉素;ACLA:阿柔比星;Piro:吡柔比星;Am:氨柔比星;Eso:依索比星;mAMSA:4’-(辣根联苯氨甲氧基苯醯腆胺);IDA:伊达比星均为抗肿瘤抗生素。
试验二、抗肿瘤抗生素的体内抑瘤作用
以大白鼠为试验对象,将2x105个肿瘤细胞皮下注射于其季肋部,待肿瘤生长14天后将其分为以下10组(见表2)。第一组为对照,第2到10组为治疗组,其中,第2组为伊达比星(IDA),第3到6组分别为mDox(7-O-甲基诺加-4’-表阿霉素)、ACLA(阿柔比星)、Am(氨柔比星)和mAMSA(4’-(辣根联苯氨甲氧基苯醯腆胺)。第7到10组分别为IDA与BCNU、ACNU、CCNU及雌莫司的联合。所有药物均经瘤内注射,剂量为5mg/kg。治疗后第30天测量肿瘤体积大小,比较治疗效果(见表2)。
表2
| 试验组(n) | 所受治疗 | 肿瘤体积(cm<sup>3</sup>) | P值 |
| 1(6) | 对照 | 78.5±23cm<sup>3</sup> | |
| 2(6) | IDA | 62±4.3cm<sup>3</sup> | <0.05 |
| 3(6) | mDox | 50±2.5cm<sup>3</sup> | <0.01 |
| 4(6) | ACLA | 40±3.6cm<sup>3</sup> | <0.01 |
| 5(6) | Am | 42±4cm<sup>3</sup> | <0.01 |
| 6(6) | mAMSA | 42±3.8cm<sup>3</sup> | <0.01 |
| 7(6) | IDA+mDox | 22+3.6cm<sup>3</sup> | <0.001 |
| 8(6) | IDA+ACLA | 20±3.6cm<sup>3</sup> | <0.001 |
| 9(6) | IDA+Am | 20±3.6cm<sup>3</sup> | <0.001 |
| 10(6) | IDA+mAMSA | 18±3.6cm<sup>3</sup> | <0.001 |
IDA、mDox、ACLA、Am(氨柔比星)和mAMSA均为抗肿瘤抗生素。由表中结果可以看出,不同抗肿瘤抗生素也可相互增效。
试验三、抗肿瘤抗生素的体内抑瘤作用。
以大白鼠为试验对象,将2 x 105个肿瘤细胞(肝癌)皮下注射于其季肋部,待肿瘤生长14天后将其分为以下10组(见表3)。第一组为对照,第2到10组为治疗组,其中,第2到6组分别为奥柔比星、表柔比星、依索比星、伊达比星和流柔比星。第7到10组分别为奥柔比星与表柔比星、依索比星、伊达比星和流柔比星的联合。所有药物均经瘤内注射,剂量为5mg/kg。治疗后第30天测量肿瘤体积大小,比较治疗效果(见表3)。
表3
| 试验组(n) | 所受治疗 | 肿瘤体积(cm<sup>3</sup>) | P值 |
| 1(6) | 对照 | 80±21cm<sup>3</sup> | |
| 2(6) | 奥柔比星 | 54±5cm<sup>3</sup> | <0.05 |
| 3(6) | 表柔比星 | 48±2.5cm<sup>3</sup> | <0.01 |
| 4(6) | 依索比星 | 44±3.2cm<sup>3</sup> | <0.01 |
| 5(6) | 伊达比星 | 48±3.6cm<sup>3</sup> | <0.01 |
| 6(6) | 流柔比星 | 40±3.8cm<sup>3</sup> | <0.01 |
| 7(6) | 奥柔比星+表柔比星 | 30±3.2cm<sup>3</sup> | <0.001 |
| 8(6) | 奥柔比星+依索比星 | 34±3.6cm<sup>3</sup> | <0.001 |
| 9(6) | 奥柔比星+伊达比星 | 22±3.2cm<sup>3</sup> | <0.001 |
| 10(6) | 奥柔比星+流柔比星 | 20±3.4cm<sup>3</sup> | <0.001 |
试验四、不同途径抗代谢类药物的体内抑瘤作用比较。
以大白鼠为试验对象,将2x105个肿瘤细胞皮下注射于其季肋部,待肿瘤生长14天后将其分为以下10组(见表4)。第一组为对照,第2到10组为治疗组,其中,第2到4组为奥柔比星,第5到7组为表柔比星,第8到10组为依索比星。药物分别经腹腔注射(ip)、瘤内注射(it)和瘤内放置(itp)。剂量均为5mg/kg。治疗后第10天测量肿瘤体积大小,比较治疗效果(见表4)。
表4
| 试验组(n) | 所受治疗 | 肿瘤体积(cm<sup>3</sup>) | P值 |
| 1(6) | 对照 | 88±2 | |
| 2(6) | 奥柔比星(ip) | 48±5.3 | <0.05 |
| 3(6) | 奥柔比星(it) | 58±2.3 | <0.01 |
| 4(6) | 奥柔比星(itp) | 56±3.4 | <0.01 |
| 5(6) | 表柔比星(ip) | 48±3.0 | <0.01 |
| 6(6) | 表柔比星(it) | 44±3.0 | <0.01 |
| 7(6) | 表柔比星(itp) | 33±3.0 | <0.001 |
| 8(6) | 依索比星(ip) | 32±3.6 | <0.001 |
| 9(6) | 依索比星(it) | 24±3.6 | <0.001 |
| 10(6) | 依索比星(itp) | 18±3.6 | <0.001 |
以上试验结果表明,所用各种抗肿瘤抗生素在该浓度时对肿瘤细胞生长均有明显的抑制作用,但以局部用药效果较为明显,其中局部放置最为明显。局部放置植入剂不仅能够有效地抑制肿瘤生长,而且能够显著降低药物的全身毒性反应。类似增效作用还见于其它抗肿瘤抗生素。说明具有普遍意义。因此,本发明所述的抗癌药物组合物的有效成分为本发明所选任意一种(或多种)抗肿瘤抗生素。
含有以上有效成分的抗癌药物组合物可制成任意剂型或形状,但以植入缓慢释放剂为优选。
本发明抗癌药物组合物的制备方法如下:
1.将称重的药用辅料放入容器中,加一定量的有机溶剂溶解均匀,有机溶剂的量不严格限定,以充分溶解为宜。
2.加入称重之抗癌有效成份重新摇匀。药物与药用辅料的用量比例因具体要求而定。
3.去除有机溶剂。真空干燥或低温干燥法均可。
4.将干燥后的固体组合物根据需要制成各种形状。
5.分装后射线灭菌(射线剂量因体积而异)备用。也可用其它方法灭菌。
(四)具体实施方式
下面通过实施例对本发明做进一步说明,但不限于此。
实施例1:
将90mg分子量为20000的聚乳酸(PLA)放入容器中,加100毫升二氯甲烷溶解混匀后,加入10mg抗癌有效成份(奥柔比星),重新摇匀后真空干燥去除有机溶剂。将干燥后的固体组合物立即成形,分装后射线灭菌,得到含10%奥柔比星的抗癌药物组合物。
实施例2:
如实施例1所述,所不同的是所含抗癌有效成分为:
(a)1%—50% 7-O-甲基诺加-4’-表阿霉素、阿柔比星、阿克拉霉素-B、氨柔比星、4’-(辣根联苯氨甲氧基苯醯腆胺)、4-去甲氧道诺红菌素、地托比星、表柔比星、依索比星、卡柔比星、伊达比星、罗多比星、流柔比星、美多比星、奈莫柔比星、多柔比星、吡柔比星、吡柔比星、奥柔比星、2-[4-(7-氯-2-喹喔啉基氧苯氧基]-丙酸、佐柔比星或N-(2-氯乙烷)-N-亚硝基脲基柔红霉素;或
(b)1%—50%洛撒蒽醌、洛索蒽醌、吡罗蒽醌、替洛蒽醌、癌霉素、派来霉素、硫酸派来霉素、抗生素1588、波外定、盐酸阿可达佐、阿可达佐、克大霉素、乙酰克大霉素、阿佐霉素、蛇形菌素、三铁阿霉素、二乙氧醋酰阿霉素、环霉素、消癌菌素、嗜癌素、嗜癌霉素、瘤菌素、治癌菌素、重氮霉素、大菌素、大菌霉素、丙氨菌素或丙氨肽霉素;或
(c)1%—50%阿乐盖、新丝菌素、大分子霉素、新塞那霉素、诺卡菌素、诺卡菌红素、诺卡型霉素、诺加霉素、丝裂红素、多粘菌素E、吡利霉素、地红霉素、安曲霉素、恶溶菌素、达佐霉素、橄榄霉素、链黑霉素、链黑霉素甲酯、链脲霉素、培洛霉素、嘌罗霉素、司帕霉素、他利霉素、羟硝氨糖环素、蒽霉素、甲基蒽霉素、艾菲地可宁或曲林菌素;或
(d)1%—50%(盐酸)卡米诺霉素、他利霉素、巨毛霉素、去甲柔毛霉素、氯脲霉素、色霉素A3、氯佐星、去甲利福平、蒽环霉素-A、黑他七霉素、脱氧助间型霉素、嘌呤霉素、盐酸嘌呤霉素、雷查霉素、瑞必克霉素、桑霉素、抗癌霉素、西伯利亚霉素、他利霉素、米托佐罗、硒唑呋喃、斯潘格宁、盐酸锗螺胺、锗螺胺、螺妙斯定或抗癌锑。
以上均为重量百分比。
实施例3:
将90mg分子量为20000的聚乙醇酸和羟基乙酸的共聚物(PLGA)放入容器中,加100毫升二氯甲烷溶解混匀后,加入10mg抗癌有效成份(伊达比星),重新摇匀后真空干燥去除有机溶剂。将干燥后的固体组合物立即成形,分装后射线灭菌,得到含10%伊达比星的抗癌药物组合物。将抗癌药物组合物防于小白鼠皮下,定时取出测药物含量,根据剩余药物量,并计算累计释放百分数(%)。结果发现,药物在30天内均匀释放80-95%。
以上均为重量百分比。
实施例4:
如实施例3所述,所不同的是所含抗癌有效成分为:
(a)1%—50% 7-O-甲基诺加-4’-表阿霉素、阿柔比星、阿克拉霉素-B、氨柔比星、4’-(辣根联苯氨甲氧基苯醯腆胺)、4-去甲氧道诺红菌素、地托比星、表柔比星、依索比星、卡柔比星、伊达比星、罗多比星、流柔比星、美多比星、奈莫柔比星、多柔比星、吡柔比星、吡柔比星、奥柔比星、2-[4-(7-氯-2-喹喔啉基氧苯氧基]-丙酸、佐柔比星或N-(2-氯乙烷)-N-亚硝基脲基柔红霉素;或
(b)1%—50%洛撒蒽醌、洛索蒽醌、吡罗蒽醌、替洛蒽醌、癌霉素、派来霉素、硫酸派来霉素、抗生素1588、波外定、盐酸阿可达佐、阿可达佐、克大霉素、乙酰克大霉素、阿佐霉素、蛇形菌素、三铁阿霉素、二乙氧醋酰阿霉素、环霉素、消癌菌素、嗜癌素、嗜癌霉素、瘤菌素、治癌菌素、重氮霉素、大菌素、大菌霉素、丙氨菌素或丙氨肽霉素;或
(c)1%—50%阿乐盖、新丝菌素、大分子霉素、新塞那霉素、诺卡菌素、诺卡菌红素、诺卡型霉素、诺加霉素、丝裂红素、多粘菌素E、吡利霉素、地红霉素、安曲霉素、恶溶菌素、达佐霉素、橄榄霉素、链黑霉素、链黑霉素甲酯、链脲霉素、培洛霉素、嘌罗霉素、司帕霉素、他利霉素、羟硝氨糖环素、蒽霉素、甲基蒽霉素、艾菲地可宁或曲林菌素;或
(d)1%—50%(盐酸)卡米诺霉素、他利霉素、巨毛霉素、去甲柔毛霉素、氯脲霉素、色霉素A3、氯佐星、去甲利福平、蒽环霉素-A、黑他七霉素、脱氧助间型霉素、嘌呤霉素、盐酸嘌呤霉素、雷查霉素、瑞必克霉素、桑霉素、抗癌霉素、西伯利亚霉素、他利霉素、米托佐罗、硒唑呋喃、斯潘格宁、盐酸锗螺胺、锗螺胺、螺妙斯定或抗癌锑。
以上均为重量百分比。
实施例5:
如实施例1或3所述,所不同的是所用药用辅料分别为下列之一或组合:
a)分子量为5000-15000、10000-20000、25000-35000或30000-50000的聚乳酸(PLA);
b)分子量为5000-15000、10000-20000、25000-35000或30000-50000的聚乙醇酸和羟基乙酸的共聚物(PLGA);
c)乙烯乙酸乙烯酯共聚物(EVAc);
d)对羧苯基丙烷(p-CPP)与葵二酸(SA)的共聚物(聚苯丙生),对羧苯基丙烷:葵二酸重量比为10:90、20:80、30:70、40:60、50:50或60:40。
实施例6:
将80mg聚苯丙生(对羧苯基丙烷:葵二酸重量比为30:70)放入容器中,加100毫升二氯甲烷溶解混匀后,加入20mg多柔比星,重新摇匀后真空干燥去除有机溶剂。将干燥后的固体组合物立即成形,分装后射线灭菌,得到抗癌药物组合物含重量百分比20%多柔比星。将含药复合物放于小白鼠皮下,定时取出测药物含量,根据剩余药物量,并计算累计释放百分数(%)。结果发现,药物在30天内均匀释放90-95%。
实施例9:
如实施例6所述,所不同的是所含有效成分为:
(a)1%—50% 7-O-甲基诺加-4’-表阿霉素、阿柔比星、阿克拉霉素-B、氨柔比星、4’-(辣根联苯氨甲氧基苯醯腆胺)、4-去甲氧道诺红菌素、地托比星、表柔比星、依索比星、卡柔比星、伊达比星、罗多比星、流柔比星、美多比星、奈莫柔比星、多柔比星、吡柔比星、奥柔比星、2-[4-(7-氯-2-喹喔啉基氧苯氧基]-丙酸、佐柔比星或N-(2-氯乙烷)-N-亚硝基脲基柔红霉素;或
(b)1%—50%洛撒蒽醌、洛索蒽醌、吡罗蒽醌、替洛蒽醌、癌霉素、派来霉素、硫酸派来霉素、抗生素1588、波外定、盐酸阿可达佐、阿可达佐、克大霉素、乙酰克大霉素、阿佐霉素、蛇形菌素、三铁阿霉素、二乙氧醋酰阿霉素、环霉素、消癌菌素、嗜癌素、嗜癌霉素、瘤菌素、治癌菌素、重氮霉素、大菌素、大菌霉素、丙氨菌素或丙氨肽霉素;或
(c)1%—50%阿乐盖、新丝菌素、大分子霉素、新塞那霉素、诺卡菌素、诺卡菌红素、诺卡型霉素、诺加霉素、丝裂红素、多粘菌素E、吡利霉素、地红霉素、安曲霉素、恶溶菌素、达佐霉素、橄榄霉素、链黑霉素、链黑霉素甲酯、链脲霉素、培洛霉素、嘌罗霉素、司帕霉素、他利霉素、羟硝氨糖环素、蒽霉素、甲基蒽霉素、艾菲地可宁或曲林菌素;或
(d)1%—50%(盐酸)卡米诺霉素、他利霉素、巨毛霉素、去甲柔毛霉素、氯脲霉素、色霉素A3、氯佐星、去甲利福平、蒽环霉素-A、黑他七霉素、脱氧助间型霉素、嘌呤霉素、盐酸嘌呤霉素、雷查霉素、瑞必克霉素、桑霉素、抗癌霉素、西伯利亚霉素、他利霉素、米托佐罗、硒唑呋喃、斯潘格宁、盐酸锗螺胺、锗螺胺、螺妙斯定或抗癌锑。
以上均为重量百分比。
Claims (3)
1.一种抗癌药物组合物,包括抗癌有效成分和药用辅料,其特征在于,该药物组合物是缓释剂,所述的药用辅料是缓释辅料,抗癌有效成分为抗肿瘤抗生素,组分如下:
(a)10%的伊达比星和90%的分子量为20000的聚乳酸和聚乙醇酸共聚物;或
(b)20%的多柔比星和80%的对羧苯基丙烷与癸二酸的共聚物,对羧苯基丙烷:癸二酸重量比为30:70;
以上均为重量百分比。
2.根据权利要求1所述的抗癌药物组合物,其特征在于该抗癌组合物是适合瘤内或瘤周放置的剂型。
3.权利要求1所述的抗癌药物组合物的应用,用于制备治疗起源于动物中枢神经系统、肾脏、肝、胆囊、头颈部、口腔、皮肤、粘膜、腺体、血管、骨组织、淋巴结、肺脏、食管、胃、眼睛、鼻咽部、子宫、卵巢、膀胱、结肠或直肠的原发或继发的癌或肉瘤的药物。
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Citations (5)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN1088777A (zh) * | 1992-12-18 | 1994-07-06 | 丛繁滋 | 用于癌病灶直接给药的化疗药物制剂的制备方法 |
| CN1363394A (zh) * | 2001-11-22 | 2002-08-14 | 黄石李时珍药业集团武汉李时珍药业有限公司 | 羟基喜树碱聚乳酸纳米粒的制备方法 |
| CN1410056A (zh) * | 2002-10-29 | 2003-04-16 | 浙江大学 | 一种水溶性抗癌药物微球的制备方法 |
| CN1466464A (zh) * | 2000-07-28 | 2004-01-07 | ס����ҩ��ʽ���� | 癌症治疗药 |
| WO2004075904A1 (en) * | 2003-02-26 | 2004-09-10 | Pharmacia Italia Spa | Method for treating liver cancer by intrahepatic administration of nemorubicin |
-
2004
- 2004-11-22 CN CNB2004100360978A patent/CN100464783C/zh not_active Expired - Fee Related
Patent Citations (5)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN1088777A (zh) * | 1992-12-18 | 1994-07-06 | 丛繁滋 | 用于癌病灶直接给药的化疗药物制剂的制备方法 |
| CN1466464A (zh) * | 2000-07-28 | 2004-01-07 | ס����ҩ��ʽ���� | 癌症治疗药 |
| CN1363394A (zh) * | 2001-11-22 | 2002-08-14 | 黄石李时珍药业集团武汉李时珍药业有限公司 | 羟基喜树碱聚乳酸纳米粒的制备方法 |
| CN1410056A (zh) * | 2002-10-29 | 2003-04-16 | 浙江大学 | 一种水溶性抗癌药物微球的制备方法 |
| WO2004075904A1 (en) * | 2003-02-26 | 2004-09-10 | Pharmacia Italia Spa | Method for treating liver cancer by intrahepatic administration of nemorubicin |
Non-Patent Citations (2)
| Title |
|---|
| 抗肿瘤药物临床应用的现状与研究进展. 杨春娥等.国外医药抗生素分册,第25卷第1期. 2004 |
| 抗肿瘤药物临床应用的现状与研究进展. 杨春娥等.国外医药抗生素分册,第25卷第1期. 2004 * |
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