CN100400036C - 胃肠复合型胶囊及其制备方法和应用 - Google Patents
胃肠复合型胶囊及其制备方法和应用 Download PDFInfo
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- CN100400036C CN100400036C CNB2004100548493A CN200410054849A CN100400036C CN 100400036 C CN100400036 C CN 100400036C CN B2004100548493 A CNB2004100548493 A CN B2004100548493A CN 200410054849 A CN200410054849 A CN 200410054849A CN 100400036 C CN100400036 C CN 100400036C
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- enteric solubility
- capsules
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Abstract
一种将口服药物分别在胃内和肠道内分别释放的新型制剂,涉及药品及其生产方法。该种制剂包括能在胃中溶解的胃溶囊帽(5)和能在肠道中溶解的肠溶胶囊(1、2),将在胃中释放的药物和在肠道中释放的药物分别装于(4)和(3)中,口服后胃溶囊帽先在胃中溶解,将药物(4)释放在胃中;肠溶胶囊在胃中不溶解,在肠道中溶解,将药物(3)释放在肠道中,见摘要附图。该制剂的特点:可避免药物的相互作用,提高复方药物制剂的稳定性;可控制药物在胃内和肠道内的定位释放,达到二次释放药物及延长药物释放的目的;减少某些药物对胃肠的刺激性;发挥复方药物的协同作用;并且可使药物的成分及含量检测更加简单、有效、准确。
Description
一、技术领域
本发明涉及一种胃肠复合型胶囊及其制备方法和应用。该胶囊口服后分别在胃内和肠道内释放药物,该胶囊由胃溶型材料制成的囊帽和肠溶性胶囊组成。
二、背景技术
目前口服药物剂型很多,包括片剂、胶囊剂、口服液、丸剂、乳剂等,但其释放药物部位大多单一在胃或者在肠道,存在以下缺点:①单点释放药物会加重胃或肠道损伤,例如给药剂量为10mg,而胃肠道不良反应的阈剂量为5mg,若按照传统的剂型给药,必然会增加不良反应的发生率;②传统剂型血药浓度波动范围较大,药物峰浓度可能会引起中毒;③药物作用时间短,服药次数多;④复方制剂中给药时间难以确定,例如格列吡嗪要求饭前30分钟给药,盐酸二甲双胍要求进餐时或进餐后给药,二者复方制剂何时给药比较合理是常规制剂难以解决的问题。⑤按照传统方法,药物理化性质不稳定,或易于发生相互作用的药物很难制成复方制剂;⑥由于复方药物之间的相互作用,药物有效期可能缩短。⑦传统复方制剂由于几种药物混合存在,给制剂的质量控制引入诸多麻烦。
目前存在一些复合胶囊剂型,如多层药用胶囊(授权公告号CN 2614676Y);分隔式药物胶囊(授权公告号CN 2423892Y);护卫丹胶囊(授权公告号CN 2506254Y);复合胶囊(授权公告号CN 2601094Y)。多层胶囊、护卫丹胶囊、复合胶囊都属于大胶囊里面套小胶囊,胶囊体积较大,胶囊空间载药量降低,病人难以服用,而且都没有采用胶囊胃肠包衣技术,无法实现药物分别在胃内和肠道内分别释放。分隔式药物胶囊虽然胶囊体积较小,但是无法应用胶囊胃肠包衣技术,无法实现药物分别在胃内和肠道内分别释放。
三、发明内容
本发明所要解决的技术问题是提供一种实现在胃内和肠道内分别释放的胃肠复合型胶囊,其特征在于由胃溶型材料制成的囊帽和肠溶性胶囊组成。
胃溶型材料制成的囊帽由胃溶型材料组成,胃溶型材料选自明胶,动物胶或其它蛋白质成分的一种或其混合物。肠溶性胶囊是由肠溶型材料组成,肠溶型材料选自虫胶、醋酸纤维素酞酸酯、丙烯酸树脂类(如Eudragit L和S型等)、聚醋酸乙烯苯二甲酸酯、邻苯二甲酸羟丙甲纤维素酯、琥珀酸醋酸羟丙甲基纤维素、以及增塑剂(如邻苯二甲酸二乙酯、聚乙二醇、丙二醇、甘油三乙酸酯、邻苯二甲酸二甲酯、癸二酸二丁酯、柠檬酸三乙酯、柠檬酸三丁酯、乙酰基柠檬酸三乙酯、蓖麻油和各种百分比的乙酰化单酸甘油酯、甘油、苯二甲酸二甲酯、苯二甲酸二乙酯、苯二甲酸二丁酯、枸橼酸三乙酯、枸橼酸三丁酯、乙酰基枸橼酸三丁酯、乙酰基枸橼酸三丁酯等)与致孔剂(如PEG类、PVP、蔗糖、盐类)等一种或其混合物。胶囊材料还可以加入各种着色剂与避光剂(二氧化钛等)。
胃肠复合型胶囊的应用方法,包含如下步骤:①制备胃溶型材料制成的囊帽和肠溶性胶囊,②机械灌装药物,主要工序包括肠溶性胶囊的供给,肠溶性胶囊胶壳排列,校准方向,肠溶性胶囊胶壳分离,在肠溶性胶囊中填充药物,③肠溶性胶囊胶壳闭合,④在胃溶型材料制成的囊帽中填充药物,闭合,送出。肠溶性胶囊和胃溶型材料制成的囊帽的闭合可以采用凹槽式锁合、明胶带密封、加热密封、化学密封等方法。胃溶型材料制成的囊帽和肠溶性胶囊中可以填充同一种药物或复方药物或各种药剂学可用的赋形剂和辅料,分别在胃部和肠道释放。其中胃溶型材料制成的囊帽和肠溶性胶囊中可以装入固体颗粒、片剂、胶囊、滴丸、微丸或液体制剂,装药量小于500mg。
胃溶型材料制成的囊帽中所装的药物为:格列吡嗪、格列奇特、格列美脲、格列苯脲、格列喹酮、瑞格列奈、罗格列酮、匹格列酮、阿卡波糖、伏格列波糖、辛伐他汀、阿托伐他汀、罗伐他汀、依那普利、赖诺普利、苯那普利、氯沙坦、依贝沙坦、丹参滴丸、六味地黄丸、金丝桃素或苦瓜素。其中胃溶型材料制成的囊帽中还可以使用多种赋形剂和辅料等,所述的赋形剂和辅料包含淀粉、微晶纤维素、无机盐类、羟丙基甲基纤维素、乙基纤维素、聚丙烯酸树脂类、聚羧乙烯类、海藻酸的可溶性/不溶性盐类、十八醇、十八酸、蔗糖、糊精、乳糖、糖粉、葡萄糖、氯化钠、半胱氨酸、柠檬酸和亚硫酸钠等的一种或几种物质的组合物。
肠溶性胶囊中所装的药物为:阿司匹林、对乙酰氨基酚、吲哚美辛、舒林酸、萘普生、双氯芬酸、萘丁美酮、洛索洛芬、尼美舒利、炎痛喜康、美洛昔康、塞莱昔布、罗非昔布、布洛芬、四环素、多西环素、红霉素、琥乙红霉素、罗红霉素、阿奇霉素、克拉霉素、麦白霉素、麦迪霉素、乙酰螺旋霉素、甲硝唑、氨甲喋呤、6-疏基嘌呤、5-氟脲嘧啶、促肾上腺皮质激素、糖皮质激素、二甲双胍、利血平、酚妥拉明、甲磺丁脲、咖啡因、甲状腺素、氨茶碱、雌激素、巯甲丙脯酸或维生素。其中肠溶性胶囊中还可以使用多种赋形剂和辅料等,所述的赋形剂和辅料包含淀粉、微晶纤维素、无机盐类、羟丙基甲基纤维素、乙基纤维素、聚丙烯酸树脂类、聚羧乙烯类、海藻酸的可溶性/不溶性盐类、十八醇、十八酸、蔗糖、糊精、乳糖、糖粉、葡萄糖、氯化钠、半胱氨酸、柠檬酸和亚硫酸钠等的一种或几种物质的组合物。
胃肠复合型胶囊在体内释药可按以下机理进行:
a)释药,胃溶型材料制成的囊帽在胃液的酸性作用下水解,囊帽破坏,药物释放到胃内。肠溶性胶囊在胃液的酸性环境中不溶解,在肠液的碱性作用下水解,胶囊溶解,药物释放到肠道中。
b)转运,胃内释放的药物由于颗粒比较小,很快排空到肠道,而肠溶性胶囊部分体积比较大,排空到肠道时间比较慢,大约延迟30分钟~1小时。
c)吸收和药理作用,胃内释放的药物在胃和小肠很快吸收,肠道内释放的药物吸收较慢。两种药物的吸收峰值分离,使得药理作用温和。图1表示服用胃肠复合型胶囊后,药理效应强度(如:血压、血糖等);图2表示服用一般胶囊后,药理效应强度(如:血压、血糖等)。由图可以看出胃肠复合型胶囊药理作用温和、作用时间延长、毒副作用降低。
与传统口服制剂相比胃肠复合型胶囊的优点在于:①减少胃肠道损伤,使药物在胃与肠道中分别释放,既达到了临床药理作用,又不引起胃肠道的不良反应,增加了病人的顺应性;②由于在胃内释放的药物吸收时间与在肠道内释放的药物吸收时间相差30分钟~1小时,使血药浓度波动范围减小;③药物吸收时间延长,有一定的缓释效应,减少病人服药次数;④使复方药物给药时间更为合理化,胃内释放的药物比肠道内释放的药物提前30分钟~1小时到达肠道;⑤利用该制剂手段可以将理化性质不稳定的药物制成复方制剂;⑥可以延长药物有效期,减少由于复方药物之间相互作用引起的药物失效。
胃肠复合型胶囊的制备:生产肠溶性胶囊囊帽,在囊帽内侧做成卡口;生产肠溶性胶囊囊体,在胶囊体两端分别做成卡口;生产胃溶型材料制成的囊帽,在囊帽内侧做成卡口。按现有技术生产肠溶性胶囊,然后再把胃溶型材料制成的囊帽卡在肠溶性胶囊囊体的末端。见图3
在得到胃溶型材料制成的囊帽和肠溶性胶囊后,填充药物,进行机械灌装,主要工序包括肠溶胶囊的供给,肠溶性胶囊胶壳排列,校准方向,肠溶性胶囊胶壳分离,在肠溶性胶囊中填充药物,肠溶性胶囊胶壳闭合,在胃溶型材料制成的囊帽中填充药物,闭合,送出。其中肠溶性胶囊和胃溶型材料制成的囊帽的闭合可以采用凹槽式锁合、明胶带密封、加热密封、化学密封等方法。一般可采用传统的囊帽和囊体的锁沟套合技术,使囊帽和囊体的锁沟相互吻合,从而保证囊体和囊帽可靠的密封,锁沟的深浅可根据需要加以调整。为了进一步保证制剂的稳定,可使用明胶带密封,或在交接处将囊帽与囊体融合在一起,或使用低共溶点液体,通过化学反应密封囊帽和囊体。具体的工业生产操作流程简图见图4。
该种制剂由于将两种活性药物分别填充在胃溶型材料制成的囊帽和肠溶性胶囊中,便于质量控制,使两种药物的分析检测更加简单,准确。
四、附图说明
图1、服用胃肠复合型胶囊后的血糖下降值;
图2、服用普通胶囊后的血糖下降值;
图3、胃肠复合型胶囊设计工艺;
图4、胃肠复合型胶囊工业化生产设计;
图5、胃肠复合型胶囊的结构示意图。图中:1、肠溶性胶囊囊帽;2、肠溶性胶囊囊体;3、肠道内释放的药物;4、胃内释放的药物;5、胃溶型材料制成的囊帽;
图6、丹参滴丸阿司匹林胃肠复合型胶囊制剂;
图7、格列吡嗪二甲双胍胃肠复合型胶囊制剂;
图8、复方二甲双胍胃肠复合胶囊制剂在胃液和肠液中的释放曲线;
图9、普通二甲双胍片的体外释放曲线;
图10、复方阿司匹林胃肠复合胶囊制剂的体外溶出曲线;
图11、普通复方阿司匹林的体外溶出曲线;
图12、复方双嘧达莫胃肠复合胶囊制剂体外溶出曲线;
图13、普通双嘧达莫体外溶出曲线。
五、具体实施方式
实施例1胃肠复合型胶囊制备及应用方法1
胃溶型材料制成的囊帽:应用明胶、二氧化钛、着色剂为材料,热融后在特定模具中倒模干燥而成。
肠溶性囊体:应用明胶为主要材料制备普通胶囊,并制备肠溶包衣液进行包衣,具体包衣液组方如下:
丙烯酸树脂II号和丙烯酸树酯III号各2份,蓖麻油2g,邻苯二甲酸二乙酯2g,吐温802g,95%乙醇加至100ml。
生产工艺:将胃溶胶囊在模具上成模后再蘸一次肠溶包衣液,进行脱模、切口、套合、即成肠溶型空心胶囊。
得到上述胃溶型材料制成的囊帽和肠溶性囊体后,机械灌装药物,主要工序包括肠溶性胶囊的供给,肠溶性胶囊胶壳排列,校准方向,肠溶性胶囊分离,在肠溶性胶囊中填充药物,肠溶性胶囊胶壳闭合,在胃溶型材料制成的囊帽中填充药物,用凹槽式锁合方式闭合,送出。
实施例2胃肠复合型胶囊制备及应用方法2
肠溶性胶囊制备如下:称取丙烯酸树脂L型1份,药用明胶10份,蒸馏水30份,配制成水溶性胶液,加入1%~2%邻苯二甲酸二乙酯,1%PVP,0.5%色素后,用特制囊模蘸胶一次制成基础胶囊,干燥后,囊外再蘸取一次8%的肠溶型丙烯酸树脂水溶液即得。
得到上述胃溶型材料制成的囊帽和肠溶性囊体后,机械灌装药物,主要工序包括肠溶性胶囊的供给,肠溶性胶囊胶壳排列,校准方向,肠溶性胶囊胶壳分离,在肠溶性胶囊中填充药物,肠溶性胶囊胶壳闭合,在胃溶型材料制成的囊帽中填充药物,用凹槽式锁合方式闭合,送出。
实施例3丹参滴丸阿司匹林胃肠复合型胶囊制剂。
处方组成:
胃溶性部分 丹参滴丸 6粒
肠溶性部分 阿司匹林 75mg
淀粉 75mg
微分硅胶 2%
生产工艺取阿司匹林与淀粉采用等量递加稀释法混合均匀后,以5%PVP乙醇溶液为粘合剂,采用湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得。
体外溶出方法按照中国药典2000版2部附录XC第二法溶出度测定法测定,体外溶出曲线:参考图6:
实施例4格列吡嗪二甲双胍胃肠复合型胶囊制剂。
处方的组成:
胃溶性部分 格列吡嗪 2.5mg
十二烷基硫酸钠 1%
淀粉 45mg
微粉硅胶 2%
生产工艺取格列吡嗪与十二烷基硫酸钠和淀粉采用等量递加稀释法混合均匀后,以5%PVP水溶液为粘合剂,采用湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得。
肠溶胶囊部分 盐酸二甲双胍 250mg
淀粉 50mg
微粉硅胶 2%
生产工艺取盐酸二甲双胍与淀粉采用等量递加稀释法混合均匀后,以5%PVP水溶液为粘合剂,采用湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得灌装即得。
参考图7:
体外溶出方法按照中国药典2000版2部附录XC第二法溶出度测定法测定,体外溶出曲线:参考图8、图9。
实施例5复方阿司匹林胃肠复合型胶囊制剂。
处方组成:
胃溶部分 单硝酸异山梨酯 20mg
淀粉 30mg
微粉硅胶 2%
生产工艺取单硝酸异山梨酯与淀粉采用等量递加稀释法混合均匀后,以5%PVP乙醇溶液为粘合剂,湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得。
肠溶性部分 阿司匹林 75mg
淀粉 75mg
微分硅胶 2%
生产工艺取阿司匹林与淀粉采用等量递加稀释法混合均匀后,以5%PVP乙醇溶液为粘合剂,采用湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得。
体外溶出方法按照中国药典2000版2部附录XC第二法溶出度测定法测定,溶出曲线:参考图10、图11。
实施例6复方双嘧达莫胃肠复合型胶囊制剂
处方组成:
胃溶部分 双嘧达莫 25mg
淀粉 25mg
微分硅胶 2%
生产工艺取双嘧达莫和淀粉采用等量递加稀释法混合均匀后,以5%PVP乙醇溶液为粘合剂,湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得。
肠溶性部分 阿司匹林 75mg
淀粉 75mg
微分硅胶 2%
生产工艺取阿司匹林与淀粉采用等量递加稀释法混合均匀后,以5%PVP乙醇溶液为粘合剂,采用湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得。
体外溶出方法按照中国药典2000版2部附录XC第二法溶出度测定法测定,溶出曲线:参考图12、图13。
实施例7阿司匹林萘磺酸右丙氧芬胃肠复合型胶囊制剂。
处方组成:
胃溶部分 萘磺酸右丙氧芬 50mg
淀粉 25mg
微分硅胶 2%
生产工艺取萘磺酸右丙氧酚和淀粉采用等量递加稀释法混合均匀后,以5%PVP乙醇溶液为粘合剂,湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得。
肠溶性部分 阿司匹林 75mg
淀粉 75mg
微分硅胶 2%
生产工艺取阿司匹林与淀粉采用等量递加稀释法混合均匀后,以5%PVP乙醇溶液为粘合剂,采用湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得。
实施例8磷酸可待因阿司匹林胃肠复合型胶囊制剂。
处方组成:
胃溶部分 磷酸可待因 5mg
淀粉 45mg
微分硅胶 2%
生产工艺取磷酸可待因和淀粉采用等量递加稀释法混合均匀后,以5%PVP乙醇溶液为粘合剂,湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得。
肠溶性部分 阿司匹林 75mg
淀粉 75mg
微分硅胶 2%
生产工艺取阿司匹林与淀粉采用等量递加稀释法混合均匀后,以5%PVP乙醇溶液为粘合剂,采用湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得。
实施例9罗格列酮盐酸二甲双胍胃肠复合型胶囊制剂。
处方的组成:
胃溶性部分 罗格列酮 2.5mg
淀粉 45mg
微粉硅胶 2%
生产工艺取罗格列酮与淀粉采用等量递加稀释法混合均匀后,以5%PVP乙醇溶液为粘合剂,采用湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得。
肠溶胶囊部分 盐酸二甲双胍 250mg
淀粉 50mg
微粉硅胶 2%
生产工艺取盐酸二甲双胍与淀粉采用等量递加稀释法混合均匀后,以5%PVP水溶液为粘合剂,采用湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得灌装即得。
实施例10格列美脲盐酸二甲双胍胃肠复合型胶囊制剂。
处方的组成:
胃溶性部分 格列美脲 1mg
十二烷基硫酸钠 1%
淀粉 49mg
微粉硅胶 2%
生产工艺取格列美脲与十二烷基硫酸钠和淀粉采用等量递加稀释法混合均匀后,以5%PVP水溶液为粘合剂,采用湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得。
肠溶胶囊部分 盐酸二甲双胍 250mg
淀粉 50mg
微粉硅胶 2%
生产工艺取盐酸二甲双胍与淀粉采用等量递加稀释法混合均匀后,以5%PVP水溶液为粘合剂,采用湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得灌装即得。
实施例11辛伐他汀阿司匹林胃肠复合型胶囊制剂。
处方组成:
胃溶部分 辛伐他汀 10mg
淀粉 40mg
微分硅胶 2%
生产工艺取辛伐他汀和淀粉采用等量递加稀释法混合均匀后,以5%PVP乙醇溶液为粘合剂,湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得。
肠溶性部分 阿司匹林 75mg
淀粉 75mg
微分硅胶 2%
生产工艺取阿司匹林与淀粉采用等量递加稀释法混合均匀后,以5%PVP乙醇溶液为粘合剂,采用湿法制粒工艺,制粒,40度干燥后加入微粉硅胶混匀后灌装即得。
Claims (8)
1.一种胃肠复合型空心胶囊,其特征在于由胃溶型材料制成的囊帽和肠溶性空
心胶囊组成,胃溶型材料制成的囊帽位于肠溶性空心胶囊囊体外,肠溶性空心胶囊囊体与胃溶型材料制成的囊帽的开口端相接,形成由胃溶型材料制成的囊帽和肠溶性空心胶囊囊体封闭的空腔,药物放置在由胃溶型材料制成的囊帽和肠溶性空心胶囊囊体封闭的空腔内或肠溶性空心胶囊空腔内。
2.根据权利要求1中所述的胃肠复合型空心胶囊,其特征在于所述的胃溶型材料是明胶。
3.根据权利要求1中所述的胃肠复合型空心胶囊,其特征在于所述的肠溶性空心胶囊是由肠溶型材料制成,肠溶型材料选自虫胶、醋酸纤维素酞酸酯、丙烯酸树脂类、聚醋酸乙烯苯二甲酸酯、邻苯二甲酸羟丙甲纤维素酯或琥珀酸醋酸羟丙甲基纤维素。
4.根据权利要求2或3所述的胃肠复合型空心胶囊,其特征在于空心胶囊材料加入着色剂与避光剂。
5.权利要求1-4中任一项所述的胃肠复合型空心胶囊的制备方法:①在肠溶性囊帽内侧做成卡口;②在肠溶性胶囊体两端分别做成卡口;③生产胃溶型材料制成的囊帽,在囊帽内侧做成卡口;④把胃溶型材料制成的囊帽卡在肠溶性胶囊体的末端。
6.权利要求1-4中任一项所述的胃肠复合型空心胶囊在制备药物制剂中的用途,包含如下步骤:①制备胃溶型材料制成的囊帽和肠溶性空心胶囊,②机械灌装药物,工序包括肠溶性空心胶囊的供给,肠溶性空心胶囊胶壳排列,校准方向,肠溶性空心胶囊胶壳分离,在肠溶性胶囊中填充药物,③肠溶性胶囊胶壳闭合,④在胃溶型材料制成的囊帽中填充药物,闭合,送出。
7.根据权利要求6所述的用途,其特征在于闭合采用凹槽式锁合、明胶带密封、加热密封或化学密封方法。
8.根据权利要求6所述的用途,其特征在于胃溶型材料制成的囊帽和肠溶性空心胶囊中填充同一种药物或复方药物或药剂学可用的辅料。
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| CN102274191B (zh) * | 2011-06-10 | 2012-09-05 | 浙江丽水众益药业有限公司 | 药物组合物红霉素肠溶微丸胶囊 |
| CN102349887A (zh) * | 2011-08-02 | 2012-02-15 | 天津市嵩锐医药科技有限公司 | 双氯芬酸钠对乙酰氨基酚胃肠型胶囊药物组合物 |
| WO2013148258A1 (en) * | 2012-03-29 | 2013-10-03 | Jerome Schentag | Gastrointestinal site-specific oral vaccination formulations active on the ileum and appendix |
| AU2014239883B2 (en) | 2013-03-14 | 2019-01-17 | Therabiome, Llc | Targeted gastrointestinal tract delivery of probiotic organisms and/or therapeutic agents |
| CN104758180A (zh) * | 2014-01-06 | 2015-07-08 | 山东诚创医药技术开发有限公司 | 一种复方制剂胶囊的二次填充方法 |
| US10674899B2 (en) * | 2017-07-12 | 2020-06-09 | Capsovision Inc | Capsule enteric coating for controlling balloon expansion start time |
| CN108078988B (zh) * | 2018-02-13 | 2019-10-25 | 山西省太原晋阳制药厂 | 双氯芬酸钠与磷酸可待因复方缓释组合物及其制备方法 |
| CN112679624B (zh) * | 2021-03-18 | 2021-07-20 | 华南理工大学 | 一种生命营养胶囊 |
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| CN2423892Y (zh) * | 2000-04-30 | 2001-03-21 | 尹为民 | 分隔式药物胶囊 |
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| CN1376060A (zh) * | 1999-07-30 | 2002-10-23 | 史密丝克莱恩比彻姆有限公司 | 多组分药用剂型 |
| CN2423892Y (zh) * | 2000-04-30 | 2001-03-21 | 尹为民 | 分隔式药物胶囊 |
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