Top 5 Target	Count

Mat2A(S-adenosylmethionine synthase isoform type-2)	2
RET(Tyrosine-protein kinase receptor RET)	1
CDK7(Cyclin-dependent kinase 7)	1
CDK9 x TNIK	1
EED x PDE9A x PKR	1

Drugs associated with Sichuan Direction Pharmaceutical Co. Ltd.

Chloral Hydrate

Target-

Mechanism-

Active Org.

Chengdu Shuode Pharmaceutical Co.,Ltd. [+9]

Originator Org.-

Active Indication

Sedation

Inactive Indication-

Drug Highest PhaseApproved

First Approval Ctry. / Loc.

China

First Approval Date30 Dec 2019

Dexmedetomidine Hydrochloride

Target

ADRA2

Mechanism

ADRA2 agonists

Active Org.

BioXcel Therapeutics, Inc. [+15]

Originator Org.

Orion Oyj

Active Indication

Bipolar I disorder [+13]

Inactive Indication

Acute Ischemic Stroke [+13]

Drug Highest PhaseApproved

First Approval Ctry. / Loc.

United States

First Approval Date17 Dec 1999

Iopromide

Target

M1 receptor x M3 receptor

Mechanism

M1 receptor antagonists [+2]

Active Org.

Bayer HealthCare Pharmaceuticals, Inc. [+4]

Originator Org.-

Active Indication

Breast Diseases [+7]

Inactive Indication-

Drug Highest PhaseApproved

First Approval Ctry. / Loc.

Australia

First Approval Date12 Sep 1991

172

Clinical Trials associated with Sichuan Direction Pharmaceutical Co. Ltd.

CTR20250811

/ RecruitingPhase 3

尿素[13C]片呼气试验药盒用于诊断胃幽门螺杆菌感染的开放、随机、交叉、自身对照、多中心临床研究

[Translation] An open, randomized, crossover, self-controlled, multicenter clinical study on the use of urea [13C] breath test kit in the diagnosis of gastric Helicobacter pylori infection

评价尿素[13C]片呼气试验药盒诊断胃幽门螺杆菌感染的准确性和安全性及与参比制剂对幽门螺杆菌诊断检测结果的一致性。

[Translation]

To evaluate the accuracy and safety of the urea [13C] breath test kit in diagnosing gastric Helicobacter pylori infection and its consistency with the reference preparation in diagnosing Helicobacter pylori.

Start Date10 Apr 2025

Sponsor / Collaborator

Brilliant Pharmaceutical Co. Ltd.

CTR20250501

/ RecruitingNot Applicable

苯磺酸美洛加巴林片在健康受试者中的生物等效性试验

[Translation] Bioequivalence study of melogabalin besylate tablets in healthy volunteers

主要目的：本研究以成都倍特药业有限公司生产的苯磺酸美洛加巴林片（5mg，按C12H19NO2计）为受试制剂，持证商第一三共株式会社在日本上市的未进口原研苯磺酸美洛加巴林片（5mg，按C12H19NO2计）（商品名：Tarlige®）为参比制剂，评价受试制剂和参比制剂在空腹及餐后条件下给药的生物等效性。次要目的：观察受试制剂和参比制剂在健康受试者中的安全性。

[Translation]

Primary objective: This study used melogabalin besylate tablets (5 mg, calculated as C12H19NO2) produced by Chengdu Beite Pharmaceutical Co., Ltd. as the test preparation and the original melogabalin besylate tablets (5 mg, calculated as C12H19NO2) (trade name: Tarlige®) marketed in Japan by the licensed manufacturer Daiichi Sankyo Co., Ltd. as the reference preparation to evaluate the bioequivalence of the test preparation and the reference preparation under fasting and postprandial conditions. Secondary objective: To observe the safety of the test preparation and the reference preparation in healthy subjects.

Start Date13 Mar 2025

Sponsor / Collaborator

Brilliant Pharmaceutical Co. Ltd.

NCT06348797

/ Not yet recruitingPhase 1IIT

Phase I Clinical Study on Safety and Feasibility of DLL3 Targeted Α-PD-L1/4-1BB Modifying Chimeric Antigen Receptor T-cells in Patients with Relapsed or Refractory Small Cell Lung Cancer (SCLC)

A study to evaluate the safety and feasibility of α-PD-L1/4-1BB DLL3 Chimeric Antigen Receptor (CAR)-T (BHP01) in patients with Relapsed/Refractory Small Cell Lung Cancer (SCLC) and determine the appropriate CAR-T cell dose. Next, In dose expansion phase, patients were assign two groups with/without bridge radiotherapy.

Start Date10 Jan 2025

Sponsor / Collaborator

Sichuan University

[+1]

100 Clinical Results associated with Sichuan Direction Pharmaceutical Co. Ltd.

0 Patents (Medical) associated with Sichuan Direction Pharmaceutical Co. Ltd.

Literatures (Medical) associated with Sichuan Direction Pharmaceutical Co. Ltd.

21 Apr 2025·Cancer Research

Abstract 5611: Preclinical evaluation of SNH-110: A potent, selective, next-generation RET inhibitor overcoming adaptive drug resistances

Author: Li, Xueyu ; Yu, Zanyang ; Tang, Jun ; Tang, Yuanqing ; Zhao, Shuchun ; Wang, Jing ; Li, Zhiqiang ; Li, Nan ; Li, Min ; Wei, Xuezhen ; Zeng, Shaomei ; Wang, Liyang ; Jia, Zhiqiang ; Yong, Can

AbstractBackground:Inhibiting RET kinase is a fundamental therapeutic approach for malignancies related to RET alterations. Despite the remarkable efficacy of pralsetinib and selpercatinib in treating various cancers, resistances due to newly surfacing on-target mutations pose a challenge. The emergence of adaptive mutations at the solvent-front, such as G810C/S/R, coupled with the occurrence of concurrent mutations at both the gatekeeper and solvent front regions, render these medications ineffective. Furthermore, off-target VEGFR2 inhibition can lead to the onset or exacerbation of hypertension, frequently necessitating dose adjustments or termination, consequently hindering cancer treatment outcomes. In response to this urgent challenge, we identified SNH-110, a potent next-generation RET inhibitor.Methods:The selectivity and activity of SNH-110 were assessed via in vitro kinase assays, and its potency was evaluated using modified Ba/F3 cell lines. The in-vivo efficacy of SNH-110 was further validated in a variety of RET-driven tumor models.Results:In a comprehensive analysis of 378 kinases, SNH-110 demonstrated a level of selectivity on par with selpercatinib, but without the concerning interactions with JAKs and VEGFR2. In cellular proliferation tests, SNH-110 exhibited robust inhibition of a range of Ba/F3 cell lines expressing various RET mutations. The IC50 values indicated a significant enhancement over selpercatinib, particularly in activities related to G810 mutations. Notably, SNH-110 displayed almost 100-fold selectivity against VEGFR2 in a cellular assay, a non-RET target associated with hypertension. At the anticipated effective concentration, SNH-110 showed no inhibitory effects on JAKs, suggesting a reduced risk of lung infection side effects compared to pralsetinib. SNH-110 demonstrated impressive anti-tumor efficacy across various RET-based models. Administered in doses from 0.1 to 3 mg/kg, SNH-110 significantly reduced tumor growth in various murine models, with inhibition rates between 85-146%. In the Ba/F3 KIF5B-RET G810R model, a 3 mg/kg dose of SNH-110 resulted in an exceptional 99% tumor growth inhibition. It's worth highlighting that SNH-110's effectiveness in controlling tumor proliferation increased with the dose across these models.Conclusions:SNH-110 stands out as a powerful contender in the field of next-generation RET inhibitors. It showcases impressive efficiency in both in vitro and in vivo studies, working against a broad array of RET mutations. Importantly, it effectively combats resistance prompted by solvent front mutations, while retaining selectivity over JAKs and VEGFR2. Its remarkable potency allows for a daily dosage as low as single-digit milligrams to be effective in humans, as indicated by animal efficacy models. A submission of an IND application to the FDA and NMPA is planned for 2025.Citation Format:Shaomei Zeng, Jing Wang, Zanyang Yu, Xuezhen Wei, Xueyu Li, Can Yong, Zhiqiang Jia, Shuchun Zhao, Min Li, Liyang Wang, Nan Li, Zhiqiang Li, Yuanqing Tang, Jun Tang. Preclinical evaluation of SNH-110: A potent, selective, next-generation RET inhibitor overcoming adaptive drug resistances [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2025; Part 1 (Regular Abstracts); 2025 Apr 25-30; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2025;85(8_Suppl_1):Abstract nr 5611.

27 Mar 2025·Journal of Medicinal Chemistry

Discovery of BT-114143, a Novel and Potent Phosphoric Acid-Containing Small-Molecule Plasminogen Activation Inhibitor for Hyperfibrinolysis

Article

Author: Ji, Sen ; Zhang, Xiaodong ; Zeng, Shaomei ; Wang, Hao ; Li, Zhiqiang ; Tang, Jun ; Hu, Xiao ; Wang, Xiao ; Li, Min ; Wang, Yan ; Li, Jianzong ; Qi, Jun

Fibrinolysis, the natural process of blood clot dissolution regulated by plasmin, plays a crucial role in preserving vascular health. Nevertheless, if this process becomes hyperactive, it can lead to severe bleeding episodes, particularly in instances of traumatic injuries. Conventional antifibrinolytics such as ε-aminocaproic acid (EACA) and tranexamic acid (TXA) exhibit limited impact attributed to their modest potency. The substantial dosage volume necessary for effectiveness, along with safety concerns, especially when administered in high doses, further constrains their usage. In response to these challenges, we have engineered BT-114143, an innovative plasminogen activation inhibitor featuring a phosphoric acid functional group. Crafted through structure-based drug design and nonclassical bioisosteres, BT-114143 has demonstrated significant antifibrinolytic activity and target selectivity in extensive preclinical studies. Presently, BT-114143 is in Phase Ib clinical trials in China (CTR20222910), representing a noteworthy progression in antifibrinolytic therapy.

22 Mar 2024·Cancer Research

Abstract 2726: A novel trispecific antibody HC010 targeting PD-1/CTLA-4/VEGF for the potential treatment in anti-PD-1 antibody resistant NSCLC patients

Author: Wang, Xingding ; Li, Zhaohui ; Jiang, Diandong ; Yang, Teddy ; Yin, Qiaoshan ; Xi, Yue ; Xu, Chen

AbstractBackground and Aim: Immune checkpoint inhibitors (anti-PD-1/CTLA-4 antibody) have been approved and widely used for the first line treatment of non-small cell lung cancer (NSCLC). However, most patients are experiencing resistant to PD-1 blockade. In recent clinical trials, anti-VEGF antibody has shown to improve the clinical outcomes of anti-PD-1 antibodies and overcome resistance to checkpoint blockade. We developed a PD-1/CTLA-4/VEGF trispecific antibody (HC010) by site-specifically fusing anti-PD-1 scFv and anti-CTLA-4 nanobody to the defined site of anti-VEGF antibody. The aim of this study was to evaluate the potential use of HC010 for treatment of anti-PD-1 antibody resistant NSCLC patients.Method: Humanized mice were established in NCG mice by reconstituting human PBMC before inoculating the PDX tissue, which was derived from a NSCLC patient treated with two cycles of an anti-PD-1 antibody sintilimab. When tumors were approx. 170mm3, mice were dosed with HC010 twice weekly for 3 weeks. Pembrolizumab, sintilimab and a Standard of Care (SoC) agent docetaxel were included as reference. For IHC analysis, tumor samples were harvested 24h post final dose and fixed with 10% NFB overnight and subsequently stained with CD31 and CD8 to explore the change in tumor microenvironment after HC010 treatment. For preclinical toxicity assessment, HC010 was intravenously administered once weekly for four weeks in naïve cynomolgus monkeys and immunogenicity/local tolerance/clinical pathology were evaluated during the dosing and recovery phase.Results: HC010 showed a significant tumor inhibition (TGI=81%) when compared with the vehicle control. Pembrolizumab and sintilimab alone exhibited limited anti-tumor effect. Docetaxel only showed a partial response during the dosing phase. By analyzing tumor samples, there was a significant increase in CD8+ positive T cells in HC010 treated tumors in contrast to the vehicle group and pembrolizumab/sintilimab treated groups, suggesting that HC010 can significantly improve CD8+ T cell infiltration. Expression of CD31 as an angiogenic and vasculogenic marker, was significantly reduced in HC010 treated tumors. In the toxicity study, HC010 at selected doses showed no obvious toxicity in cynomolgus monkeys.Conclusion: Our trispecific antibody HC010 targeting PD-1/CTLA-4/VEGF showed a superior anti-tumor effect in a sintilimab resistant PDX animal model when compared with pembrolizumab and sintilimab as well as SoC. By analyzing tumor microenvironment, HC010 overcame acquired resistance by modulating tumor microenvironment such as increase in intra-tumoral cytotoxic T cell infiltration and normalization of blood vessels. Together with preclinical efficacy and safety data, HC010 showed potential benefits in treatment of anti-PD-1 antibody resistant NSCLC patients.Citation Format: Diandong Jiang, Yue Xi, Chen Xu, Xingding Wang, Qiaoshan Yin, Zhaohui Li, Teddy Yang. A novel trispecific antibody HC010 targeting PD-1/CTLA-4/VEGF for the potential treatment in anti-PD-1 antibody resistant NSCLC patients [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2024; Part 1 (Regular Abstracts); 2024 Apr 5-10; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2024;84(6_Suppl):Abstract nr 2726.

News (Medical) associated with Sichuan Direction Pharmaceutical Co. Ltd.

29 Jul 2024

·www.echemi.com

Brilliant Pharmaceutical Achieves New Success - Betamethasone Sodium Phosphate Injection Approved, 26 Products Pass Evaluation in 2023

On July 24, the official website of the State Drug Administration (NMPA) released the latest announcement that betamethasone sodium phosphate injection, a generic drug of Chengdu Brilliant Pharmaceutical Co., Ltd. has been officially approved and deemed to have passed the evaluation. This achievement marks another significant achievement for Bett Pharmaceutical in 2023. According to statistics, since the beginning of the year, Bette Pharmaceutical and its subsidiaries have successfully passed the evaluation of the number of drugs reached 26, which fully demonstrates the company's strong research and development capabilities and market competitiveness. Betamethasone sodium phosphate injection, as a glucocorticoid drug widely used in clinic, plays an important role in the treatment of allergic and autoimmune diseases, such as lupus erythematosus, rheumatoid arthritis, asthma and other chronic diseases. According to the data of pharmaceutical Rongyun, the sales of the drug in the national hospital market in 2023 has exceeded 100 million yuan, an increase of nearly 45%, and the market demand continues to maintain a strong trend. In the field of generic drugs, the production approval of betamethasone sodium phosphate injection is also extremely competitive. At present, a total of 8 domestic enterprises have obtained the production approval of the drug, of which 3 enterprises, such as Chongqing Huabang Pharmaceutical, Chengdu Brilliant Pharmaceutical and Suicheng Pharmaceutical, have successfully passed the evaluation. In addition, there are 17 enterprises are actively reporting the listing of the variety, is in the review and approval stage. In recent years, Bett Pharmaceutical has continuously committed to the enrichment and expansion of its product line, and the number of generic drug approvals has continued to hit a new high. In particular, in 2023, the company and its subsidiaries have successfully passed the evaluation of 26 drug varieties, including three important varieties with first imitation significance, such as Furosemide oral solution. These achievements not only highlight the strong strength of Brilliant Pharmaceutical in the field of research and development, but also provide more high-quality and reliable drug choices for the majority of patients. Looking forward to the future, Bette Pharmaceutical will continue to increase investment in research and development, and continue to promote the enrichment and upgrading of product pipelines. The company is committed to providing patients with better quality and more reliable medical products, and contributing its own strength to the cause of human health.

Drug Approval

100 Deals associated with Sichuan Direction Pharmaceutical Co. Ltd.

100 Translational Medicine associated with Sichuan Direction Pharmaceutical Co. Ltd.

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Pipeline

Pipeline Snapshot as of 09 May 2025

The statistics for drugs in the Pipeline is the current organization and its subsidiaries are counted as organizations,Early Phase 1 is incorporated into Phase 1, Phase 1/2 is incorporated into phase 2, and phase 2/3 is incorporated into phase 3

Discovery

Preclinical

IND Application

IND Approval

Phase 1 Clinical

Phase 2 Clinical

Phase 3 Clinical

NDA/BLA

Approved

Other

Current Projects

Drug(Targets)	Indications	Global Highest Phase

Dexmedetomidine Hydrochloride ( ADRA2 )	Sedation More	Approved
Ticarcillin Disodium	Bacterial Infections More	Approved
Aminocaproic Acid ( Plasminogen activators )	Hemorrhage More	Approved
Chloral Hydrate	-	NDA/BLA
Semaglutide biosimilar (Brilliant) ( GLP-1R )	Diabetes Mellitus, Type 2 More	Phase 3

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