主要目的：以持证商为Les Laboratoires Servier的培哚普利氨氯地平片（Ⅰ）（商品名：COVERAM，规格：每片含精氨酸培哚普利10mg和苯磺酸氨氯地平（以氨氯地平计）10mg）为参比制剂，以南京海纳制药有限公司研发的培哚普利氨氯地平片（Ⅰ）（每片含精氨酸培哚普利10mg和苯磺酸氨氯地平（以氨氯地平计）10mg）为受试制剂，评价两种制剂在中国健康受试者中空腹和餐后状态下的生物等效性。次要目的：观察受试制剂和参比制剂在中国健康受试者中的安全性。

[Translation]

Primary objective: To evaluate the bioequivalence of the two preparations in the fasting and fed state in healthy Chinese subjects, using perindopril amlodipine tablets (I) (trade name: COVERAM, specification: each tablet contains 10 mg of perindopril arginine and 10 mg of amlodipine besylate (calculated as amlodipine)) from the licensee Les Laboratoires Servier as the reference preparation and perindopril amlodipine tablets (I) (each tablet contains 10 mg of perindopril arginine and 10 mg of amlodipine besylate (calculated as amlodipine)) developed by Nanjing Haina Pharmaceutical Co., Ltd. as the test preparation. Secondary objective: To observe the safety of the test preparation and the reference preparation in healthy Chinese subjects.

Start Date05 Sep 2024

Sponsor / Collaborator

Nanjing Healthnice Pharmaceutical Co., Ltd.

CTR20242729

/ CompletedNot Applicable

培哚普利氨氯地平片（Ⅲ）在中国成年健康受试者中的一项随机、开放、空腹和餐后单次给药、两制剂、两序列、两周期交叉的生物等效性研究

[Translation] A randomized, open-label, single-dose, two-formulation, two-sequence, two-period crossover bioequivalence study of perindopril and amlodipine tablets (III) in healthy Chinese adult subjects

考察空腹/餐后单次口服受试制剂培哚普利氨氯地平片（Ⅲ）（规格：每片含精氨酸培哚普利10 mg和苯磺酸氨氯地平（以氨氯地平计）5 mg，安徽佳和药业有限公司生产）与参比制剂培哚普利氨氯地平片（Ⅲ）（商品名：Coveram®，规格：每片含精氨酸培哚普利10 mg和苯磺酸氨氯地平（以氨氯地平计）5 mg，Servier (Ireland) Industries Ltd生产），在中国成年健康人体的相对生物利用度，分析两种制剂的药代动力学参数，评价两制剂的生物等效性。次要研究目的：评价空腹/餐后单次口服受试制剂和参比制剂在中国成年健康受试者中的安全性。

[Translation]

To investigate the relative bioavailability of the test preparation perindopril amlodipine tablets (III) (specification: each tablet contains 10 mg perindopril arginine and 5 mg amlodipine besylate (calculated as amlodipine), produced by Anhui Jiahe Pharmaceutical Co., Ltd.) and the reference preparation perindopril amlodipine tablets (III) (trade name: Coveram®, specification: each tablet contains 10 mg perindopril arginine and 5 mg amlodipine besylate (calculated as amlodipine), produced by Servier (Ireland) Industries Ltd) in healthy Chinese adults after a single oral administration on an empty stomach/after a meal, analyze the pharmacokinetic parameters of the two preparations, and evaluate the bioequivalence of the two preparations. Secondary study objectives: To evaluate the safety of the test preparation and the reference preparation in healthy Chinese adults after a single oral administration on an empty stomach/after a meal.

Start Date20 Aug 2024

Sponsor / Collaborator

Anhui Jiahe Pharmaceutical Co., Ltd.Startup

CTR20242507

/ CompletedNot Applicable

培哚普利氨氯地平片（Ⅲ）在中国成年健康受试者中的一项随机、开放、空腹和餐后单次给药、两制剂、两序列、两周期交叉的生物等效性研究。

[Translation] A randomized, open-label, single-dose, fasting and postprandial, two-formulation, two-sequence, two-period crossover bioequivalence study of perindopril and amlodipine tablets (III) in healthy adult Chinese subjects.

主要研究目的：考察空腹/餐后单次口服受试制剂培哚普利氨氯地平片（Ⅲ）（规格：每片含精氨酸培哚普利10 mg和苯磺酸氨氯地平（以氨氯地平计）5 mg，海南皇隆制药股份有限公司生产）与参比制剂培哚普利氨氯地平片（Ⅲ）（商品名：Coveram®，规格：每片含精氨酸培哚普利10 mg和苯磺酸氨氯地平（以氨氯地平计）5 mg，Servier (Ireland) Industries Ltd生产），在中国成年健康人体的相对生物利用度，分析两种制剂的药代动力学参数，评价两制剂的生物等效性。次要研究目的：评价空腹/餐后单次口服受试制剂和参比制剂在中国成年健康受试者中的安全性。

[Translation]

Main study objectives: To investigate the relative bioavailability of the test preparation perindopril amlodipine tablets (III) (specification: each tablet contains 10 mg perindopril arginine and 5 mg amlodipine besylate (calculated as amlodipine), produced by Hainan Huanglong Pharmaceutical Co., Ltd.) and the reference preparation perindopril amlodipine tablets (III) (trade name: Coveram®, specification: each tablet contains 10 mg perindopril arginine and 5 mg amlodipine besylate (calculated as amlodipine), produced by Servier (Ireland) Industries Ltd) in healthy Chinese adults after a single oral administration on an empty stomach/after a meal, analyze the pharmacokinetic parameters of the two preparations, and evaluate the bioequivalence of the two preparations. Secondary study objectives: To evaluate the safety of the test preparation and the reference preparation in healthy Chinese adults after a single oral administration on an empty stomach/after a meal.

Start Date22 Jul 2024

Sponsor / Collaborator

Hainan Hualon Pharmaceutical Co., Ltd.

100 Clinical Results associated with Amlodipine Besylate/Perindopril Arginine

100 Translational Medicine associated with Amlodipine Besylate/Perindopril Arginine

100 Patents (Medical) associated with Amlodipine Besylate/Perindopril Arginine

1,009

Literatures (Medical) associated with Amlodipine Besylate/Perindopril Arginine

01 Mar 2025·Journal of Hazardous Materials

In situ self-cleaning removal of emerging organic contaminants with covalent organic framework armed with arylbiguanide

Article

Author: Tumrani, Sadam Hussain ; Qi, Ruifang ; Dong, Lili ; Lei, Jinming ; Feng, Chenghong

An in situ self-cleaning covalent organic framework featuring arylbiguanide arms (Aryl-BIG-COF) was first developed to remove emerging organic pollutants such as propranolol (PRO) from water. The main breakthroughs addressed the scarcity of functional active sites, the impracticality of ex situ regeneration, and the rapid recombination of electronhole pairs in the application of COFs. Owing to the directional capture ability and electronic structure regulation of the arylbiguanide arms, the adsorption capacity and photocatalytic degradation rate of the newly synthesized COF increased by nearly four and seven times, respectively. Its self-cleaning ability, driven by the photocatalytic regeneration of active sites, enabled in situ removal of PRO and sustained over 90 % removal efficiency after six cycles. Moreover, it demonstrated broad applicability for removing PRO and other emerging pollutants, such as bisphenol A (BPA), tetracycline (TC), and norfloxacin (NOR), across various water matrices with less residual toxicity. The coexisting organic matter and ions in natural water promoted the removal of PRO. The enhancement mechanism involved arylbiguanide arms narrowing the band gap and inducing local charge polarization, thereby increasing the separation efficiency of electronhole pairs. This work provides significant insights into the structural design and practical applications of COFs for purifying water.

01 Feb 2025·International Journal of Biological Macromolecules

Enhancing fruit preservation with sodium alginate films incorporating propolis extract and graphene oxide

Article

Author: Guo, Junyan ; Zhang, Wanli ; Khan, Mohammad Rizwan ; Ahmad, Naushad

In this work, sodium alginate (SA) composite films containing propolis extract (PRO) and graphene oxide (GO) were developed. Subsequently, the effects of PRO and GO on different properties of SA composite films were studied, and the films were characterized by scanning electron microscopy, fourier transform infrared spectroscopy, X-ray diffraction, and thermogravimetric analysis. The PRO release properties and fruit preservation performance of the developed composite films were also investigated. The results showed that the incorporation of PRO resulted in a 51.16% increase in tensile strength. The simultaneous incorporation of PRO and GO reduced water vapor permeability (WVP) by 22.56% compared to the SA film. The temperatures at which the SA/GO/PRO film lost 5% of its weight were 8.0°C higher than those of the SA film. The incorporation of GO into the SA/PRO composite film also modulates the release of PRO. Furthermore, the incorporation of PRO and GO improved the tensile strength of the SA film, as reflected in the microstructure of the films. The reduced WVP of the SA composite film allowed the packaged blueberries to exhibit less weight loss and shrinkage, thereby prolonging their shelf life.

01 Feb 2025·Journal of Human Nutrition and Dietetics

The evolution of nutritional care in children with food allergies – With a focus on cow's milk allergy

Review

Author: Venter, Carina ; Santos, Alexandra ; Meyer, Rosan ; Groetch, Marion

AbstractCow's milk allergy (CMA) remains one of the most common and complex paediatric food allergies. In the last decade, our understanding has advanced in terms of immunoglobulin E (IgE)‐mediated CMA and focus is now also paid to non‐IgE‐mediated CMA, particularly in some Western countries where incidence rates are high. We have had significant progress in the last 10 years in relation to our understanding of existing supportive tests for IgE‐mediated CMA, with the advancement of newer tests, such as the basophil activation test (BAT), which have shown great promise. However, little advancement has been made in terms of tests for non‐IgE‐mediated CMA, and controversy still exists around symptoms. Our understanding of the natural history of CMA has also advanced with more awareness of different phenotypes. While the mainstay of management remains cow's milk elimination, the importance of supporting breastfeeding and avoidance of unwarranted cow's milk elimination diets in breastfeeding mothers has been highlighted. For non‐breastfed children, there has been some advancement in the formulas offered for the management of CMA, including the recognition of hydrolysed rice‐based formulas and increased demand for nutritionally complete plant‐based options, some of which are currently being assessed. The addition of pro, pre and synbiotics is considered safe to use, although research and guidance on routine use remain absent. Knowledge of tolerance induction from studies on the early introduction of peanuts has also highlighted the importance of a more active approach to managing CMA with the use of milk ladders, primarily in non‐IgE‐mediated CMA and baked milk (BM) introduction in IgE‐mediated CMA. In addition, modulation of the microbiome and diet diversity during complementary feeding has been a major advancement in the last 10 years. While data on poor growth and feeding difficulties in children with CMA has not changed much, increased rates of obesity are now also reported. Finally, novel approaches, including oral immunotherapy, the use of milk ladders and earlier consideration of BM, have advanced somewhat in the last decade, although the risks and benefits of these novel approaches require further research. While CMA remains a complicated allergy to diagnose and manage, the evolution of science has advanced our knowledge and brought some novel innovations, which combined have enhanced our practice.

News (Medical) associated with Amlodipine Besylate/Perindopril Arginine

21 Feb 2024

·www.biospace.com

Discover this new generic drug in the PERINDOPRIL range

MONTREAL, Feb. 21, 2024 /CNW/ - Pharmascience Canada is proud to announce the launch of pms-PERINDOPRIL-AMLODIPINE (perindopril arginine and amlodipine), a drug indicated for the treatment of mild to moderate essential hypertension in adults aged 18 to 65 for whom combination therapy is appropriate. This oral treatment contains two medicines, perindopril arginine and amlodipine. They work together to control the blood pressure. pms-PERINDOPRIL-AMLODIPINE are available in bottles of 100 tablets and comes in the following dosage forms: 3.5 mg / 2.5 mg (this treatment is indicated for initial therapy in patients with mild to moderate essential hypertension.) 7 mg / 5 mg 14 mg / 10 mg This medication is a generic equivalent of Viacoram MD1. pms-PERINDOPRIL-AMLODIPINE tablets are available at affordable prices. « We are excited to introduce Perindopril Amlodipine to the Canadian market, as it reflects our mission to improve the health and quality of life of Canadians through innovative and high-quality products, » said Mike Dutton, Vice-President and General Manager of Pharmascience Canada. « Perindopril Amlodipine is manufactured in our Canadian facility which is another example of how we leverage our expertise and capabilities to deliver value to our customers and patients. » ABOUT PHARMASCIENCE INC. Founded in 1983, Pharmascience Inc. is the largest pharmaceutical employer in Quebec with 1,500 employees proudly headquartered in Montreal. Pharmascience Inc. is a full-service privately owned pharmaceutical company with strong roots in Canada and a growing global reach with product distribution in over 50 countries. Ranked 50th among Canada's top 100 Research & Development (R&D) investors in 2022, with 40-50 million dollars invested each year, Pharmascience Inc. is among the largest drug manufacturers in Canada. Pharmascience Inc. has strong values based on the importance of investing in its employees and young people. Through various programs and initiatives, the company ensures it supports their personal development and life. In 2024, the company was awarded Great Place to Work certification for the third year running. PRVIACORAM®1 is a registered trademark owned by Servier Canada Inc. For product information, please contact Pharmascience's Medical Information Department at 1-888-550-6060. SOURCE Pharmascience Inc.

Drug Approval

31 Mar 2023

·www.biospace.com

Prothena Presents New Preclinical Data Supporting Best-in-Class Profile of PRX012, a Next-Generation Anti-Amyloid Beta Antibody, at AD/PD 2023

Data from oral presentation adds to growing body of evidence supporting the pro PRX012, which is designed to target all aggregated forms of amyloid beta with high binding potency Demonstrated 20-fold higher affinity to amyloid beta soluble protofibrils when compared to lecanemab Clears pyroglutamate-modified amyloid beta at lower concentrations when compared to donanemab DUBLIN--(BUSINESS WIRE)-- Prothena Corporation plc (NASDAQ:PRTA), a late-stage clinical biotechnology company with a robust pipeline of investigational therapeutics built on protein dysregulation expertise, today announced new preclinical data from its PRX012 program, a potential best-in-class anti-amyloid beta (Aβ) product candidate in development for the treatment of Alzheimer’s disease, at the 2023 International Conference on Alzheimer’s and Parkinson’s Diseases and related neurological disorders (AD/PD) in Gothenburg, Sweden. To build a more in-depth understanding of the pro PRX012 and its potential as a best-in-class anti-Aβ treatment for Alzheimer’s disease, two preclinical studies presented in an oral presentation at AD/PD 2023 compare a PRX012-surrogate* (PRX012s) to approved and investigational molecules. Surface Plasmon Resonance (SPR) was used to compare PRX012s to lecanemab+ and showed that PRX012s had approximately 20-fold higher affinity to Aβ protofibrils as compared to lecanemab when tested under the same conditions. This result was largely driven by a slower binding dissociation rate of PRX012s versus lecanemab. The second study, an ex vivo study using post-mortem Alzheimer’s disease brain tissue, was designed to test the ability of PRX012s to clear pyroglutamate-modified Aβ deposited in plaques. Study results showed that lower concentrations of PRX012s induced more potent and robust clearance of pyroglutamate-modified Aβ as compared to donanemab+. In the experiment, microglia simultaneously phagocytosed non-pyroglutamate-modified Aβ and pyroglutamate-modified Aβ in the presence of PRX012s, indicating that high opsonization efficiency of plaques by PRX012s was sufficient to clear both forms of Aβ. “These new preclinical data add to the scientific rationale of the PRX012 program, which has the potential to deliver a next-generation Alzheimer’s disease treatment and enable a more convenient administration for patients and caregivers,” said Wagner Zago, Ph.D., Chief Scientific Officer at Prothena. “With more than 55 million people worldwide estimated to be living with Alzheimer’s disease or other dementias, the timely delivery of improved disease modifying treatments is critical for these patients and their families. Prothena is committed to delivering a patient-centric, best-in-class Aβ-targeting antibody with the potential to robustly and safely deplete Aβ plaques.” These data add to the growing body of evidence supporting the pro PRX012, which is designed to target all aggregated forms of Aβ with high binding potency. The data further support the ongoing clinical development of PRX012 as a potential best-in-class treatment for Alzheimer’s disease that could enable improved access and more convenient administration for patients and caregivers. Additional Prothena Activities at AD/DP 2023 Other activities at AD/PD 2023 showcased Prothena’s broad participation at this year's congress bringing together thought leaders in Alzheimer’s disease research, including Prothena leadership, at a company-sponsored Symposium titled Entering the Era of Disease-Modifying Treatments for AD: Taking Stock of Today and Looking to Tomorrow. Two Forum Discussions, Immunotherapies in AD: From Basics to Approval and Anti-Tau Therapies in Clinical Trials also featured Prothena’s scientific leadership. Prothena’s prasinezumab development partner Roche also contributed poster and oral presentations highlighting aspects of the Phase 2 PASADENA study of prasinezumab for the treatment of Parkinson’s disease. About PRX012 PRX012, an investigational next-generation anti-Aβ antibody, was designed as a subcutaneous IgG1 mAb to target multiple aggregated forms of Aβ, including protofibrils and plaques, with high binding affinity. PRX012 is currently being investigated in Phase 1 clinical studies for the treatment of Alzheimer’s disease. Preclinical data have demonstrated binding of PRX012 to beta amyloid plaques and oligomers with high affinity, resulting in effective Aβ plaque occupancy and removal at relatively lower antibody concentrations, potentially enabling lower volumes of administration for subcutaneous delivery. Preclinical data have also demonstrated clearance of both pyroglutamate modified and unmodified Aβ plaque in brain tissue at concentrations of PRX012 estimated to be clinically achievable in the central nervous system with subcutaneous delivery. About Alzheimer’s Disease Alzheimer’s disease is a fatal disease and the most common form of dementia causing increasingly serious symptoms, including confusion, disorientation, mood and behavioral changes, and difficulty speaking, swallowing, and walking. More than 55 million people worldwide are estimated to be living with Alzheimer’s disease or other dementias. Alzheimer’s disease is the most common neurodegenerative disorder. There is an urgent need for therapies that slow the progression and ultimately prevent Alzheimer’s disease to address this global healthcare crisis. Prothena’s Alzheimer’s disease portfolio spans next generation antibody immunotherapy, small molecule, and vaccine approaches, geared toward building upon first generation treatments to advance the treatment paradigm. About Prasinezumab Prasinezumab is a humanized monoclonal antibody that targets a carboxyl terminal epitope of alpha-synuclein, a protein found in neurons that can aggregate and spread from cell to cell, resulting in the neuronal dysfunction and loss that causes Parkinson’s disease. Prasinezumab is designed to block the cell-to-cell transmission of the aggregated, pathogenic forms of alpha-synuclein in Parkinson's disease, thereby slowing clinical decline. In December 2013, Prothena and Roche entered into a worldwide collaboration to develop and commercialize antibodies that target alpha-synuclein, including prasinezumab. For more information on the Phase 2b PADOVA clinical study of prasinezumab in patients with early Parkinson's disease, visit clinicaltrials.gov (NCT#04777331). About Parkinson's Disease Parkinson's disease is a progressive degenerative disorder of the entire nervous system that affects one in 100 people over age 60. An estimated seven to 10 million people are living with Parkinson's disease worldwide. It is the second most common neurodegenerative disorder after Alzheimer's disease. The disease is characterized by the neuronal accumulation of aggregated alpha-synuclein in the central nervous system and peripheral nervous system that results in a wide spectrum of worsening progressive motor and non-motor symptoms. While diagnosis relies on motor symptoms classically associated with Parkinson's disease, non-motor symptoms may present many years earlier. Current treatments for Parkinson's disease are symptomatic and only address a subset of symptoms such as motor impairment, dementia, or psychosis. There are currently no treatments available that target the underlying cause of the disease and can slow its progression. About Prothena Prothena Corporation plc is a late-stage clinical biotechnology company with expertise in protein dysregulation and a pipeline of investigational therapeutics with the potential to change the course of devastating neurodegenerative and rare peripheral amyloid diseases. Fueled by its deep scientific expertise built over decades of research, Prothena is advancing a pipeline of therapeutic candidates for a number of indications and novel targets for which its ability to integrate scientific insights around neurological dysfunction and the biology of misfolded proteins can be leveraged. Prothena’s pipeline includes both wholly-owned and partnered programs being developed for the potential treatment of diseases including AL amyloidosis, ATTR amyloidosis, Alzheimer’s disease, Parkinson’s disease and a number of other neurodegenerative diseases. For more information, please visit the Company’s website at and follow the Company on Twitter @ProthenaCorp. Forward-looking Statements This press release contains forward-looking statements. These statements relate to, among other things, the treatment potential, designs, proposed mechanisms of action, and potential administration of PRX012 and prasinezumab. These statements are based on estimates, projections and assumptions that may prove not to be accurate, and actual results could differ materially from those anticipated due to known and unknown risks, uncertainties and other factors, including but not limited to those described in the “Risk Factors” sections of our Annual Report on Form 10-K filed with the Securities and Exchange Commission (SEC) on February 28, 2023, and discussions of potential risks, uncertainties, and other important factors in our subsequent filings with the SEC. We undertake no obligation to update publicly any forward-looking statements contained in this press release as a result of new information, future events, or changes in our expectations. _____________________ * “Surrogate” is defined as an antibody with >99.5% homology, the same binding epitope and equivalent binding pro different forms of Aβ where directly compared. + Lecanemab and donanemab were generated from publicly available sequences.

Phase 2ImmunotherapyPhase 1License out/in

100 Deals associated with Amlodipine Besylate/Perindopril Arginine

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KEGG	Wiki	ATC	Drug Bank
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R&D Status

Approved

10 top approved records.

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Indication	Country/Location	Organization	Date
Hypertension	MY	Les Laboratoires Servier SAS	03 May 2010

Developing

10 top R&D records.

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Indication	Highest Phase	Country/Location	Organization	Date
Essential Hypertension	Phase 1	US	Symplmed Pharmaceuticals LLC	01 Feb 2012

Clinical Result

Indication

Phase

Evaluation

View All Results

Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


ESC2022	Not Applicable	Hypertension Second line	-	Perindopril/amlodipine+indapamide	(lmaaevcdbe) = 11 adverse reactions wazakzvrsm (jhvouxahxe )	-	07 Apr 2022
AVANT’AGE STUDY (ESH2018)	Not Applicable	-	378	Perindopril/Amlodipine 5/5 mg	btqwlzfxvu(byxdmxrait) = 1.5% (p < 0. 0001) esfsyhxeie (hxiwiixnrw )	Positive	01 Jun 2018
				Perindopril/Amlodipine 5/10 mg
ESH2018	Not Applicable	Hypertension \| Arteriosclerosis	-	Perindopril/amlodipine 5mg/5mg	cqtrwuyeqg(eazzsqfedo) = kujgyfpdrr tcltewuxqo (ieehpjcqiy )	Positive	01 Jun 2018
				Perindopril/amlodipine 10mg/10mg	cqtrwuyeqg(eazzsqfedo) = kjreqssvxr tcltewuxqo (ieehpjcqiy )
[PP.05.10] (ESH2017)	Not Applicable	-	1,814	Perindopril/Amlodipine 3.5/2.5 mg	raoskcrcad(hemvykwvvm) = morypcydcf ldlxnowyig (ojgvjdxnwi ) View more	Positive	01 Sep 2017
				Perindopril/Amlodipine 7/5 mg	qmftmpxjee(umdbflrhrn) = aexsqjgokd wtbqcqjqet (mvloojzdlm ) View more
EPHES TRAIL (ESH2017)	Not Applicable	-	60	Perindopril/Amlodipine 5/5 mg	wclmvydywv(jksqruluyj) = IMTmax decreased significantly only in patients with IHD tehpaomrst (yuniendqqq ) View more	Positive	01 Sep 2017
				Perindopril/Amlodipine 10/10 mg
ESC2016	Not Applicable	Hypertension	102	Perindopril/amlodipine combination	ylbalbyakq(uvkhfczhjq) = hxlxgssies bjritodfxl (amfwzxlaxn )	-	07 Dec 2016
PEARL (ESH2016)	Not Applicable	-	262	Perindopril/Amlodipine 5 mg/5 mg	nwezfolbhy(uoblnllfju) = phjrxzrqmt fmxmvggzuh (jcajqvertx, 8.9) View more	Positive	01 Sep 2016
				Perindopril/Amlodipine 5 mg/10 mg	nwezfolbhy(uoblnllfju) = uljofydyai fmxmvggzuh (jcajqvertx, 8.9) View more
PERSPECTIVA study (ESH2016)	Not Applicable	Hypercholesterolemia	701	Perindopril 5 mg/Amlodipine 5 mg	esmyaezmzx(lgmflgaquo) = Treatment was well tolerated with a similar rate of adverse events: 0.9% in the statin (+) vs 2.5% in the statin (-) groups qlikeneotg (naqjwrwuxp )	Positive	01 Sep 2016
				Perindopril 10 mg/Amlodipine 5 mg
[PP.18.08] (ESH2016)	Not Applicable	Hypertension \| Myocardial Ischemia	27	Perindopril/Amlodipine	bvjucibtst(olcxqcsmoi) = epnclcsivq rubpvqtswz (mgowxpnhgr, 2.7) View more	Positive	01 Sep 2016
[PP.26.14] (ESH2016)	Not Applicable	Coronary Artery Disease	1,907	Perindopril/amlodipine fixed dose combination	(xmqyvsceow) = ietmwknmzi nzhwbboumc (hgbozxgnjg ) View more	Positive	01 Sep 2016

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