An Open Label 52-week Study to Evaluate the Safety and Efficacy of Tegaserod Given Orally for the Treatment of Opioid-induced Constipation (OIC) in Patients With Chronic Non-cancer Pain

This study will evaluate the safety and efficacy of Tegaserod in opioid-induced constipation in patients with non-cancer pain.
Patients who enter this study PRIOR to the core study (CHTF919N2201) interim analysis receive the treatment as follows:
Patients will be randomly assigned to receive open label tegaserod 6 mg b.i.d. or tegaserod 12 mg o.d. using an allocation ratio of 1:1.
Patients who enter this study AFTER the core study interim analysis receive the treatment as follows:
Patients will be assigned to receive the selected tegaserod dose regimen (as determined by the core study interim analysis) in an open label fashion.

开始日期2007-02-01

申办/合作机构

Novartis AG

NCT00390975 / Terminated临床4期

An Open-label Pilot Trial to Assess the Effect of Tegaserod on Improvement of Gastric Emptying in Patients With Diabetic Gastroparesis and Upper Gastrointestinal Symptoms

This study will assess gastric emptying in patients with symptoms of diabetic gastroparesis treated with tegaserod over 2 weeks.

开始日期2007-01-31

申办/合作机构

Novartis AG

NCT00399659 / Terminated临床3期

A 52-week Extension to Study CHTF919N2201 to Evaluate the Safety and Efficacy of Tegaserod (6 mg b.i.d. and 12 mg o.d.) Given Orally for the Treatment of Opioid-induced Constipation (OIC) in Patients With Chronic Non-cancer Pain

This study will evaluate the safety and efficacy of Tegaserod in opioid-induced constipation (OIC) in patients with non-cancer pain.
Patients who enter this study PRIOR to the core study (CHTF919N2201) interim analysis (IA) receive the treatment as follows:
Patients on tegaserod 6 mg twice daily (b.i.d.) or 12 mg once daily (o.d.) in the core study will remain on the same dose in the extension (double-blind).
Patients on placebo during the core study will receive tegaserod 12 mg o.d. (open-label)
Patients who enter this study AFTER the core study interim analysis will receive the selected tegaserod dose regimen (open-label) determined by the core study IA.

开始日期2006-11-30

申办/合作机构

Novartis AG

100 项与替加色罗相关的临床结果

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100 项与替加色罗相关的转化医学

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100 项与替加色罗相关的专利（医药）

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项与替加色罗相关的文献（医药）

2023-09-19·International journal of molecular sciences

Small Organic Compounds Mimicking the Effector Domain of Myristoylated Alanine-Rich C-Kinase Substrate Stimulate Female-Specific Neurite Outgrowth.

Article

作者: Monica Tschang ; Suneel Kumar ; Wise Young ; Melitta Schachner ; Thomas Theis

Myristoylated alanine-rich C-kinase substrate (MARCKS) is a critical member of a signaling cascade that influences disease-relevant neural functions such as neural growth and plasticity. The effector domain (ED) of MARCKS interacts with the extracellular glycan polysialic acid (PSA) through the cell membrane to stimulate neurite outgrowth in cell culture. We have shown that a synthetic ED peptide improves functional recovery after spinal cord injury in female but not male mice. However, peptides themselves are unstable in therapeutic applications, so we investigated more pharmacologically relevant small organic compounds that mimic the ED peptide to maximize therapeutic potential. Using competition ELISAs, we screened small organic compound libraries to identify molecules that structurally and functionally mimic the ED peptide of MARCKS. Since we had shown sex-specific effects of MARCKS on spinal cord injury recovery, we assayed neuronal viability as well as neurite outgrowth from cultured cerebellar granule cells of female and male mice separately. We found that epigallocatechin, amiodarone, sertraline, tegaserod, and nonyloxytryptamine bind to a monoclonal antibody against the ED peptide, and compounds stimulate neurite outgrowth in cultured cerebellar granule cells of female mice only. Therefore, a search for compounds that act in males appears warranted.

2023-01-12·Cancer research

The RNA m6A reader YTHDF1 is required for acute myeloid leukemia progression.

Article

作者: Yun-Guang Hong ; Zhigang Yang ; Yan Chen ; Tian Liu ; Yuyuan Zheng ; Chun Zhou ; Guo-Cai Wu ; Yinhui Chen ; Juan Xia ; Ruiting Wen ; Wenxin Liu ; Yi Zhao ; Jin Chen ; Xiangwei Gao ; Zhanghui Chen

N6-methyladenosine (m6A), the most abundant modification in mRNAs, has been defined as a crucial modulator in the progression of acute myeloid leukemia (AML). Identification of the key regulators of m6A modifications in AML could provide further insights into AML biology and uncover more effective therapeutic strategies for AML patients. Here we report overexpression of YTHDF1, an m6A reader protein, in human AML samples at the protein level with enrichment in leukemia stem cells (LSCs). Whereas YTHDF1 was dispensable for normal hematopoiesis in mice, depletion of YTHDF1 attenuated self-renewal, proliferation, and leukemic capacity of primary human and mouse AML cells in vitro and in vivo. Mechanistically, YTHDF1 promoted the translation of cyclin E2 in an m6A-dependent manner. Structure-based virtual screening of FDA-approved drugs identified tegaserod as a potential YTHDF1 inhibitor. Tegaserod blocked the direct binding of YTHDF1 with m6A-modified mRNAs and inhibited YTHDF1-regulated cyclin E2 translation. Moreover, tegaserod reduced the viability of patient-derived AML cells in vitro and prolonged survival in patient-derived xenograft models. Together, our study defines YTHDF1 as an integral regulator of AML progression by regulating the expression of m6A-modified mRNAs, which might serve as a potential therapeutic target for AML.

2022-11-03·Food & function

Lactobacillus rhamnosus GG supernatant promotes intestinal mucin production through regulating 5-HT4R and gut microbiota.

Article

作者: Yu Gu ; Xiali Qin ; Guoqiong Zhou ; Chen Wang ; Chenlu Mu ; Xiang Liu ; Weilong Zhong ; Xin Xu ; Bangmao Wang ; Kui Jiang ; Jinghua Liu ; Hailong Cao

Lactobacillus rhamnosus GG (LGG) is a well-known probiotic widely used in foods and drugs. It has been reported that LGG can improve bowel dysfunction in gastrointestinal motility disorders, such as constipation; however, the specific mechanisms remain unclear. The colonic mucus layer is mainly composed of mucin secreted by goblet cells, which plays important roles in lubricating colonic contents and maintaining normal defecation function. It has been reported that increased mucin production is beneficial for relieving constipation symptoms. In this study, we aimed to investigate the role of LGG in regulating intestinal mucin production and the associated mechanisms. Six-week-old C57BL/6J mice were randomized into 3 groups, and were treated with De-Man Rogosa and Sharpe broth (MRS group), tegaserod maleate (tegaserod group) and LGG supernatant (LGGs group) by gavage, respectively. After treatments, defecation parameters, intestinal mucin-2 (MUC2) and serotonin 4 receptor (5-HT4R), goblet cells, and microbiota composition of the mice in each group were assessed. In comparison with the MRS group, higher fecal water content and increased fecal pellet number were found in the tegaserod group and LGGs group. Moreover, LGGs increased the number of goblet cells and upregulated the expression of 5-HT4R and MUC2 in the mouse colon. In addition, Alcian Blue Periodic acid Schiff staining showed that activated 5-HT4R enhanced intestinal MUC2 secretion. Further exploration of the mechanism discovered that LGGs upregulated intestinal S100A10, which was found to be involved in regulating 5-HT4R expression. Furthermore, gut microbiota analysis showed the higher abundance of Alistipes, Allobaculum, Desulfovibrio, and Clostridium XlVa in the LGGs group, which have been reported to be involved in regulating gut motility and the intestinal barrier, and alleviating bowel dysfunction. Interestingly, gut dysbiosis was present in the tegaserod group. It is noteworthy that the fecal microbiota transplanted from LGGs-treated mice significantly improved the gut dysmotility in a constipation mouse model. Our results suggested that LGGs could upregulate 5-HT4R to promote MUC2 production, as well as modulate the gut microbiota, thus improving the defecation function in mice. This finding might provide evidence for the application of diet supplementary LGG in relieving gastrointestinal motility disorders.

项与替加色罗相关的新闻（医药）

2024-03-05

·精准药物

含吲哚药物结构与靶点，药理与SAR 研究归纳

吲哚是一种芳香杂环分子，具有一个苯环和一个含氮吡咯环组成的双环结构。吲哚中的氮原子提供一对孤对电子，形成共轭体系，从而稳定了吲哚结构。这对孤电子使吲哚化合物呈现弱碱性(pKa=16.2和pK,=17.6)。由于吡咯环的电子密度相对较高以及氮原子的共轭效应，吲哚可以在其吡咯环的3位发生亲电取代反应(图la)。图 1 (a) 全球有超过70种含有吲哚的合成药物在市场上销售，并被证明具有良好的医疗效果(图1b)。用于治疗的疾病包括糖尿病、癌症、白血病、丙型肝炎、心理障碍和其他临床问题。自2015年起，美国(FDA)专门批准了14种含吲哚药物，其中3种是在2021年批准的(图2)。二氢麦角胺(DHE,1)的化学结构中含有吲哚支架，对头颅血管平滑肌中的5-HT1b受体具有激动活性，治疗偏头痛。昂丹司琼(2)是一种血清素5-HT3受体拮抗剂，用于预防癌症治疗期间和手术后的恶心和呕吐(图3a)。图 3 (a) 双氢麦角胺（1）和昂丹司琼（2）的结构。(b) 双氢麦角胺(1)与其靶点（左）和昂丹司琼(2)与其靶点（右）的关键靶点相互作用。替加色罗(3)在临床相关水平上被认为是5-HT(4)受体的激动剂和5-HT(2B)受体的拮抗剂，其作用之一是使受损的胃肠道运动恢复正常。多拉司琼(4)用于中度致吐的癌症化疗以及术后恶心和呕吐的治疗(图5)。它是一种高效、选择性的血清素5-HT3受体拮抗剂。 Tropisetron（5）可抑制5HT3受体上血清素的活性，从而抑制放疗和化疗引起的呕吐。 Vilazodone(6)是5HT-1A受体的部分激动剂，专门抑制中枢神经系统对血清素的再摄取。在治疗偏头痛急性发作方面，三苯氧胺药物(5-羟色胺受体激动剂)比其他药物更有效、更耐受。这类药物具有起效快、用药时间长、不良反应少等优点。Sumatriptan(7),zolmitriptan(8),naratriptan(9), rizatriptan(10), almotriptan (11), frovatriptan (12), eletriptan (13), 和 oxitriptan (14) 是国外已商业化的曲坦类药物的代表。(图7)。环氧化酶(COX)被称为前列腺素G/H合成酶，而吲哚美辛是一种非特异性的可逆性环氧化酶抑制剂。吲哚美辛(18)属于吲哚-3-乙酸类，其官能团包括对氯苯甲酰基、甲基和甲氧基。它是一种非甾体抗炎药(NSAID), 具有消炎、镇痛和解热的特点(图11a)。 Acemetacin(19)是另一种强效非甾体抗炎药物，由吲哚-3-乙酸衍生而来(图12)。它主要通过酯分解代谢为吲哚美辛。 Etodolac(20)是一种非甾体抗炎药，具有消炎、镇痛和解热作用(图13a)。以前被认为是一种非选择性COX抑制剂，但现在被认为对COX-2的选择性是COX-1的5-50倍。 Carprofen(21)是兽医用作缓解老年犬关节炎症状的辅助疗法的一种非甾体抗炎药，人们认为卡洛芬(21)的作用机制是抑制环氧化酶的活性。帕金森病的药物 Cabergoline(22)是一种长效多巴胺受体激动剂，与D2受体有很强的亲和力，用于治疗高催乳素血症和帕金森综合症(图14a)。 Lisuride(23)可能是某些血清素受体的激动剂,也可能是多巴胺D1受体的拮抗剂。可降低催乳素水平，适量服用可阻止偏头痛，从药理上讲，(23)是还是一种帕金森氏症药物。治疗子宫脱垂的药物甲基麦角新碱(26)是一种麦角生物碱，临床上用于预防和治疗产后和流产后出血(图17)。这种药物与多巴胺D1受体结合，作为一种拮抗剂发挥作用，可增强平滑肌的张力、节奏和节律性收缩的幅度。治疗精神疾病的药物 sertindole（27）是一种抗精神分裂症药物，也是一种苯基吲哚衍生物。临床试验证实，(27)对低水平的多巴胺D2占位具有疗效。治疗神经系统疾病的药物吲哚洛尔(28)是一种非选择性β肾上腺素受体拮抗剂，用于治疗心房颤动、水肿、高血压和室性心动过速。卡维地洛(29)通过阻断β肾上腺素受体防止运动引起的心动过速，它对α-1肾上腺素能受体的作用可使血管平滑肌放松，从而降低外周血管阻力和血压。尼麦角林(30)是一种半合成麦角衍生物，可用于治疗认知功能障碍。这种药剂作为一种选择性α-1A肾上腺素能受体抑制剂用于临床(图20)。治疗生殖系统疾病的药物麦角新碱(32)是一种麦角生物碱，可用于控制妇女的产后和流产后出血。结构与活性关系明确的药物 Tezacaftor(41)属于用于治疗囊性纤维化(CFTR)增效剂。美国食品及药物管理局批准该药与ivacaftor联合用于治疗囊性纤维化(图28a)。该药物可在2至4小时内达到血浆浓度峰值。 2015年2月23日，FDA批准口服去乙酰化酶(DAC)抑制剂Panobinostat(42)用于治疗多发性骨髓瘤(图29a)。(42)在体外与人体血浆蛋白的结合率约为90%,这与其浓度无关。其吲哚环可以通过与Asn645的氢键相互作用为SAR创造一个稳定的框架(图29b)。结构与活性关系不完全明确的药物 Metergoline(52)是一种麦角衍生物，用于治疗女性高催乳素闭经症(图39)。通过靶向钠通道而非5HT受体来抑制钠通道的活性，从而导致泌乳素分泌减少。 Lurbinectedin(53)是一种抗癌天然产物。该药物在化疗中用于治疗转移性小细胞肺癌。Lurbinectedin(53)在临床试验中的治疗反应率和持续时间在2020年获得了加速批准。总体而言，在FDA批准的药物中，含有吲哚环的药物数量在不断增加。在药物分子中引入吲哚砌块也已成为药物化学和药物设计中的一种常见策略。现有的含吲哚药物因其特殊的结构，在抗癌、抗炎和抗病毒等方面具有显著的临床价值。参考文献：DOI: 10.1039/d3md00677h 内容来源于网络，如有侵权，请联系删除。

上市批准放射疗法

2023-09-26

·BioPharmaDive

Intercept, after biotech rollercoaster ride, agrees to buyout by Alfasigma

Liver drug developer Intercept Pharmaceuticals has agreed to be acquired by Italian company Alfasigma for about $800 million, the companies announced Tuesday, ending one of biotechnologys most noteworthy stories of investor exuberance and clinical disappointment in the last decade.Alfasigma will pay Intercept investors $19 per share in cash, an 82% premium from Intercepts closing price on Monday. Alfasigma will fund the transaction with cash on hand and corporate credit facilities, and expects to close the deal by the end of 2023.With the acquisition, Alfasigma will gain Ocaliva, a drug that treats the rare autoimmune disorder primary biliary cholangitis, or PBC, which had sales of $152 million in the first six months of the year. The company recorded losses of $38 million over the same period.Alfasigma executives said the transaction will help it develop its U.S. presence. Intercept represents a compelling fit with Alfasigmas core business areas of gastroenterology and hepatology, and we believe that the transaction represents a transformational opportunity for both companies, said Alfasigma CEO Francesco Balestrieri in a statement.A closely held company controlled by the family of its founder, Alfasigma markets drugs like Zelnorm and rifaximin for irritable bowel syndrome and sulodexide for post-thrombotic syndrome. It also provides contract manufacturing services, as well as nutritional supplements. Its factory in Shreveport, Louisiana,manufactures nutritional supplements for the U.S. market.While Ocalivafirst gained approval for PBC, the drugs potential in the liver disease NASH drove investor enthusiasm in Intercept. NASH, or non-alcoholic steatohepatitis, is a disease connected with obesity, and its believed to be growing widely in prevalence.In 2014, a National Institutes of Health Phase 2 study of Ocaliva in people with NASH was stopped early because it had met its primary goal improvement in disease activity score at an interim analysis. Shares in the company nearly quadrupled in value and took the companys valuation to more than $7 billion, sparking an investor rush to find other companies working on NASH drugs.The path to regulators was not straightforward, however. Intercept reported positive Phase 3 data in 2019, but the FDA asked for longer-term data,rejectingIntercepts first NASH application.The FDA turned back a second application earlier this year, as Ocalivas only modest benefit was balanced against signs of liver damage experienced by some trial participants given the drug. Following that rejection, Intercept canceled all work in NASH, claiming it wasnt economically feasible to collect the data asked for by the FDA, and laid off staff.Meanwhile, competition in Intercepts established market of PBC may be emerging, as CymaBays seladelpar and Genfits elafibranor near key milestones.Raymond James analyst Steven Seedhouse described the transaction as a great return for Intercept investors.Given our bullish view of seladelpar and its ability to take market share in PBC beginning as early as late 2024, it isnt clear to us if [Ocaliva] will even generate that much net profit in the next ~10 years, Seedhouse wrote in a note to clients. '

临床结果并购临床2期上市批准临床3期

2023-05-16

·蒲公英Ouryao

超过百个国产1类新药获批，恒瑞、豪森等领跑

转自：人民日报健康客户端2003年2月1日至2023年5月15日，近20年国内有百余款国产1类（含1/1.1类）新药国内获批上市，集中在全身用抗感染药物、抗肿瘤和免疫调节剂两大治疗领域。从企业获批情况看，恒瑞医药以12个品种领跑，豪森药业、先声药业以5个品种紧接在后，复星医药、中国生物制药均拿下4个品种。此外，人福医药、百济神州、和黄医药、再鼎医药、海正药业等均有3个品种获批。恒瑞医药：“创新药一哥”，12款一类创新药上市素有“创新药一哥”之称的恒瑞医药，目前已有12款创新药（11款一类新药）在国内获批上市，11款通过谈判纳入全国医保目录，其中瑞维鲁胺片、羟乙磺酸达尔西利片、脯氨酸恒格列净片3款1类新药已纳入2022版国家医保目录。羟乙磺酸达尔西利片是中国首个自主研发的新型高选择性CDK4/6抑制剂，联合氟维司群用于激素受体阳性、人表皮生长因子受体2阴性的经内分泌治疗后进展的复发或转移性乳腺癌的治疗。脯氨酸恒格列净片是中国首个自主研发的SGLT2抑制剂，用于改善成人2型糖尿病患者的血糖控制。瑞维鲁胺片是中国首个自主研发的新型雄激素受体抑制剂，用于高瘤负荷的转移性激素敏感性前列腺癌患者的治疗。瑞维鲁胺已获得《中国临床肿瘤学会（CSCO）前列腺癌诊疗指南（2022版）》I级推荐。豪森药业：5款一类创新药上市，均进入国家医保目录豪森药业已发展成为国内知名的创新型医药产业集团。截至目前，共有5款一类创新药在国内获批上市。2014年，豪森药业首款1类新药吗啉硝唑氯化钠注射液获批上市，是全球40年来首个硝基咪唑类抗厌氧菌创新药物。经过几年的沉寂，自2019年开始，豪森药业相继收获聚乙二醇洛塞那肽注射液、甲磺酸氟马替尼片、甲磺酸阿美替尼片、艾米替诺福韦片等重磅创新药。目前，豪森药业已上市的5款创新药均已进入国家医保目录，市场处于快速放量阶段。先声药业：5款一类创新药上市，多个为一线药物先声药业是最早布局创新药的企业之一，从2006年上市的血管内皮抑制素抗癌新药“重组人血管内皮抑制素注射液”，再到2011年上市的自身免疫性疾病治疗药物“艾拉莫德片”，先声药业已逐步建立起创新药物研发管线，和持续实现商业化的产品梯队。截至目前，先声药业已上市产品中拥有5款一类创新药，分别为重组人血管内皮抑制素注射液、艾拉莫德片、依达拉奉右莰醇注射用浓溶液、恩沃利单抗注射液和先诺特韦片/利托那韦片组合。其中，重组人血管内皮抑制素注射液从2017年起被纳入国家医保药品目录，被国家卫健委、中华医学会及中国临床肿瘤学会发布的多个肿瘤临床实践指南推荐作为晚期非小细胞肺癌患者的一线治疗药物。艾拉莫德从2017年起被纳入国家医保药品目录，被国家卫健委、中华医学会等许多临床实践指南及路径推荐作为治疗活动性类风湿关节炎的主要治疗药物。复星医药：4款一类创新药上市，一款10亿元以上销售额复星医药是一家以从事医药制造业为主的企业。截至目前，共有4款一类创新药，分别为盐酸凯普拉生片、斯鲁利单抗注射液、阿兹夫定片和马来酸替加色罗片。据2022年公司披露的财报显示，合作开发的新冠口服药阿兹夫定片取得了10亿元以上的年销售额。除了新冠相关的产品，PD-1斯鲁利单抗上市首年也实现3-5亿元的营收。虽然错过了国内PD-1的第一波红利，但是通过适应症的选择，H药“斯鲁利单抗”占据了市场的空白，其首个适应症MSI-H实体瘤至今仍是尚未开发的蓝海。复星医药又选中小细胞肺癌（SCLC）这一前景广阔的市场，并打败O药、K药，成为全球首个获批用于一线治疗广泛期小细胞肺癌的靶向PD-1单抗药品。中国生物制药：4款一类创新药上市，一款领跑超10亿元榜单中国生物制药有限公司是一家综合性兼集团化制药企业。截至目前，共有4款一类创新药获批上市，分别为艾贝格司亭α注射液、派安普利单抗注射液、盐酸安罗替尼胶囊和甲磺酸加替沙星氯化钠注射液。其中，明星产品盐酸安罗替尼胶囊2022年获批第五个适应症分化型甲状腺癌，以40.48亿元的销售额领跑2022年超10亿元品种榜首。百济神州：3款一类创新药上市并实现商业化百济神州成立于2010年，是我国首家实现“N+H+A”三地上市的生物制药公司。截至目前，百济神州共有泽布替尼、替雷利珠单抗、帕米帕利3款一类创新药成功上市并实现商业化。其中，泽布替尼和替雷利珠单抗是百济神州的“拳头产品”。泽布替尼主要用于治疗套细胞淋巴瘤、华氏巨球蛋白血症、边缘区淋巴瘤等的。该药于2019年通过美国食品药品监督管理局的“优先评审”率先在美国上市，成为我国第一个获得FDA批准的抗肿瘤创新药；2020年6月，该药又获得国家药品监督管理局批准在国内上市，并于同年进入国家医保目录。百济神州的另一核心自研产品替雷利珠单抗，对MSI-h或dmmR实体瘤、二线食管鳞癌、复发转移性鼻咽癌等多种癌症均有良好效果。人福医药：3款一类创新药上市，打破30年镇静药领域无创新药局面人福医药成立于1993年，是国内麻醉镇痛药龙头。截至目前，共3款一类创新药上市，分别为注射用磷丙泊酚二钠、注射用苯磺酸瑞马唑仑和注射用加替沙星。其中，注射用苯磺酸瑞马唑仑是湖北省首个化药1类新药，打破了国内外镇静药物领域近30年无创新药上市的局面；注射用磷丙泊酚二钠是公司第二款1类新药，是中国首款丙泊酚前体药物，也是目前国内外最先进的全身静脉麻醉药之一。和黄医药：3款一类创新药上市，均已纳入国家医保目录和黄医药是中国首家专注于全球市场的创新型医药研发企业之一。截至目前，共将3款一类创新药推向上市，分别为呋喹替尼、索凡替尼和赛沃替尼。呋喹替尼于2018年在国内获批上市，用于复发难治性结直肠癌的三线治疗，2020年1月起被纳入中国国家医保药品目录。索凡替尼于2021年1月在国内获批上市，用于晚期非胰腺神经内分泌瘤的治疗；2021年6月，第2项适应症获批，用于晚期胰腺神经内分泌瘤的治疗。2022年1月，索凡替尼被纳入国家医保目录。赛沃替尼于2021年6月获批用于治疗MET14号外显子跳跃突变的晚期非小细胞肺癌患者，2023年3月1日起，赛沃替尼纳入国家医保目录。再鼎医药：3款一类创新药获批上市再鼎医药是是一家拥有从早期药物发现、临床研发、生产到商业化能力的全面整合的生物制药公司。截至目前，共3款一类创新药上市，分别为注射用甲苯磺酸奥马环素、甲苯磺酸奥马环素片和甲苯磺酸尼拉帕利胶囊。尼拉帕利是再鼎医药的拳头产品，是全球首个获批用于所有铂敏感复发卵巢癌患者维持治疗，也是再鼎的第一款商业化产品，于2016年引进自TESARO（后被GSK收购），获得尼拉帕利在中国市场的独家研发和销售权。海正药业：3款一类创新药获批上市浙江海正药业是一家致力于全球化的专业制药企业。截至目前，共3款一类创新药上市，分别为注射用甲苯磺酸奥马环素、甲苯磺酸奥马环素片和海博麦布片。其中，海博麦布片通过国家药监局突破性治疗药物优先审评，于2021年上市，是公司自主研发的1类新药、中国首个口服肠道胆固醇吸收抑制剂，填补国内该领域药物空白。

上市批准CSCO会议免疫疗法

100 项与替加色罗相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
D02730	替加色罗	A06AX06	DB01079

研发状态

适应症	最高研发状态	国家/地区	公司
肠易激综合征	批准上市	南非更多	-
便秘型肠易激综合征	撤市	美国更多	Alfasigma USA, Inc. 更多
消化不良	终止	美国更多	Novartis AG 更多
胃食管反流	终止	美国更多	Novartis AG 更多
阿片类药物引起的便秘	终止	新加坡更多	Novartis Pharma AG 更多