This study will examine the effects of Tirzepatide (TZP), a glucagon-like peptide 1 (GLP1) - gastric inhibitory peptide (GIP) co-agonist, on metabolism in type 1 diabetes (T1D). Research participants with T1D will undergo measures of insulin sensitivity, and hormone levels post-meal, post-hypoglycemia and during the overnight period. These measures will be performed prior to, and after 4 weeks of treatment with TZP. These measures will also be compared to a group of adults without diabetes (who will not receive treatment with TZP) to assess how metabolism of energy and nutrients is different in T1D compared to people without diabetes.

Start Date01 Dec 2025

Sponsor / Collaborator

The Garvan Institute of Medical Research

NCT06651177

/ Not yet recruitingPhase 2IIT

NIDA CTN-0152: Evaluation of Tirzepatide As an Adjunct to Buprenorphine for the Treatment of Opioid Use Disorder: a Pragmatic, Multi-site, Double-blind, Randomized, Placebo-controlled Trial (TAB)

The primary objective of this research study is to evaluate the effect of tirzepatide, relative to placebo, as an adjunct to BUP on retention, substance use, and sleep outcomes in individuals with OUD.

Start Date16 Sep 2025

Sponsor / Collaborator

University of Cincinnati (Ohio)

[+1]

NCT06759701

/ Not yet recruitingEarly Phase 1IIT

Pre-surgical Tirzepatide-assisted Weight Loss in Men with Diabetes and Prostate Cancer: a Pilot Feasibility Study

The goal of this clinical research study is to determine how well a tirzepatide-assisted weight loss program works before a prostatectomy in patients with intermediate risk prostate cancer

Start Date30 Jun 2025

Sponsor / Collaborator

The University of Texas MD Anderson Cancer Center

100 Clinical Results associated with Tirzepatide

100 Translational Medicine associated with Tirzepatide

100 Patents (Medical) associated with Tirzepatide

676

Literatures (Medical) associated with Tirzepatide

31 Dec 2025·Journal of Pharmaceutical Policy and Practice

Compounded glucagon-like peptide-1 receptor agonists for weight loss: the direct-to-consumer market in Colorado

Article

Author: Saseen, Joseph J. ; Dardouri, Mouna ; Nair, Kavita V. ; Moore, Gina D. ; DiStefano, Michael J.

Background:

High prices and other access barriers have contributed to the rise of a market for compounded glucagon-like peptide-1 receptor agonists for weight loss in the United States. This market has not been systematically studied. We conducted a pilot study to assess the prevalence, characteristics, and advertising content of direct-to-consumer providers of compounded glucagon-like peptide-1 products for weight loss in Colorado.

Methods:

We conducted a cross-sectional study of websites advertising compounded glucagon-like peptide-1 products for weight loss in Colorado. Websites were identified using Google searches focused on census-defined statistical areas. Searches were conducted between March 21 and April 12, 2024. Data collected from websites included physical addresses, business type, highest reported staff credential, advertised glucagon-like peptide-1 products, whether businesses referred to Food and Drug Administration approval when describing products, and whether businesses referred to products as 'generic'.

Results:

We identified 93 business websites advertising compounded glucagon-like peptide-1 products for weight loss corresponding to 188 physical locations throughout Colorado. Most businesses were self-categorized as medical/health spas (33/93) or weight loss services (26/93). Advertised products included semaglutide (92/93), tirzepatide (40/93), liraglutide (2/93), and retatrutide (1/93). Advertised combination products included B vitamins (8/93), levocarnitine (1/93), mannitol (1/93), BPC-157 (1/93), and glycine (1/93). Seven websites advertised oral formulations. Additionally, 41/93 websites referred to Food and Drug Administration approval in their descriptions of compounded products and 5/93 referred to products as 'generic'.

Conclusion:

This study identified several instances of unapproved glucagon-like peptide-1 products being compounded and advertised in Colorado. Additionally, 1 product was advertised as compounded with BPC-157, a substance determined by the Food and Drug Administration to be unsafe for compounding. This study also identified numerous examples of misleading claims regarding the regulatory status of compounded glucagon-like peptide-1 products. Regulatory action is needed to ensure the benefits of compounded GLP-1 products outweigh the risks.

01 Apr 2025·CURRENT PROBLEMS IN CARDIOLOGY

Real-world efficacy of tirzepatide in patients with heart failure without diabetes

Review

Author: Kaelber, David ; Augusto, Silvio Nunes ; Tang, W H Wilson

BACKGROUND:

Tirzepatide, a dual agonist of glucose-dependent insulinotropic polypeptide (GIP) and glucagon-like peptide-1 (GLP-1) receptors, has shown significant cardiovascular benefits in clinical trials. This study investigates the real-world impact of tirzepatide on heart failure (HF) outcomes, leveraging data from the TriNetX platform.

METHODS:

Using data from January 1, 2013, to December 01, 2024, we conducted a propensity-matched analysis of two cohorts of patients with HF without diabetes, where the only difference was the use of tirzepatide. The primary outcome was the incidence of acute heart failure (acute HF), with secondary outcomes including major adverse cardiovascular events (MACE), chronic kidney disease (CKD), stroke, and coronary arterial disease (CAD).

RESULTS:

After propensity-matching, 897 patients were compared between the two cohorts in a 4-year follow-up, showing that untreated patients were at higher risk of incident acute HF (HR: 3.12, 95%CI = 2.240-4.349, log-rank p<0.001) and MACE (HR: 3.57, 95%CI = 2.32-5.48, log-rank p<0.001). Stroke (HR: 2.796, 95%CI = 1.353-5.776, log-rank p<0.01), CKD (HR: 1.48, 95%CI: 1.08-2.03, log-rank p=0.015), and CAD (HR: 1.474, 95%CI,1.169-1.859, log-rank p=0.001) outcomes also favored the treatment cohort.

CONCLUSION:

Tirzepatide presents a promising therapeutic option for managing heart failure, with significant metabolic and cardiovascular benefits. These real-world findings reinforce its potential role as a transformative treatment in improving clinical outcomes and quality of life for patients with HF without diabetes.

04 Mar 2025·Expert Review of Endocrinology & Metabolism

Association between glucagon-like peptide-1 agonists and risk of diabetic retinopathy: a disproportionality analysis using FDA adverse event reporting system data

Article

Author: Nim, Dwividendra Kumar ; Natt, Navreet Kaur ; Singh, Harmanjit

BACKGROUND:

Glucagon-like peptide-1 (GLP-1) agonists are commonly prescribed for type 2 diabetes mellitus (T2DM). Concerns have emerged regarding their potential link to diabetic retinopathy (DR).

METHODS:

To evaluate the association between GLP-1 agonists and DR, a disproportionality analysis was conducted using FDA Adverse Event Reporting System (FAERS) data from Q4/2003 to Q2/2024 via OpenVigil 2.1 software. We focused on GLP-1 agonists and glucose-dependent insulinotropic polypeptide (GIP) agonist: Semaglutide, liraglutide, dulaglutide, lixisenatide, and tirzepatide, as primary suspect drugs. 'Diabetic retinopathy' was the key search term mapped to Medical Dictionary for Regulatory Activities (MedDRA) Lower-Level Terms (LLTs). We calculated Proportional Reporting Ratio (PRR) and Reporting Odds Ratio (ROR), with 95% confidence intervals (CI) and the Evans' criteria were applied to check the significant associations.

RESULTS:

Semaglutide (PRR: 19.43, 95% CI: 15.17-24.88; ROR: 19.48, 95% CI: 15.20-24.96; Chi-square: 1078.08) and dulaglutide (PRR: 9.01, 95% CI: 7.11-11.42; ROR: 9.02, 95% CI: 7.11-11.44; Chi-square: 478.31) showed a strong association with DR. Tirzepatide and liraglutide showed a weaker but significant association while lixisenatide showed no significant association.

CONCLUSION:

GLP-1 agonists (except lixisenatide) were found to be associated with DR. These findings emphasize the need for close monitoring and further research to clarify these associations.

1,089

News (Medical) associated with Tirzepatide

02 Mar 2025

·synapse.patsnap.com

Sale of GLP-1 Small Molecule to Eli Lilly, Chugai Pharmaceutical Discloses Latest KRAS Macrocyclic Patent

Last year belonged to the realm of Pfizer's COVID-19 small molecule treatments, while this year is dominated by GLP-1 injectable and oral therapies. The tremendous popularity of GLP-1 has propelled Novo Nordisk and Eli Lilly to reach market capitalizations of 500 and 600 billion US dollars respectively. Eli Lilly emerges as the biggest winner, not only does it have the GLP-1/GIP dual agonist Tirzepatide (brand name Mounjaro) approved in the US for weight reduction indications, but it also has a GLP-1 small molecule drug Orforglipron advancing in Phase III clinical trials. Transaction information for Orforglipron in the synapse database Upon searching the Synapse database for the keyword "Orforglipron," a transaction was identified. The transaction occurred on September 26, 2018, between Eli Lilly and Company and Chugai Pharmaceutical Co., Ltd. of Japan. According to the terms of the agreement, Eli Lilly acquired the global rights to develop and commercialize OWL833 (Orforglipron). In return, Chugai received an upfront payment of $50 million and is eligible to receive milestone payments upon the achievement of certain predetermined milestones. Furthermore, if Orforglipron is successfully commercialized, Chugai will also be entitled to royalties for patent usage. At the time, Orforglipron was in the preclinical stage. In comparison with the $185 million upfront payment that Chengyi Biologics received from AstraZeneca, Chugai indeed sold the asset at a relatively low price. Chugai Pharmaceutical is a member of the Roche Group (with Roche currently holding 59.89% of Chugai's shares), yet it maintains autonomous and independent management, employing a unique business model focused on innovation that values individuality and diversity. Chugai's alliance with Roche provides it with the exclusive rights to market Roche's innovative pharmaceutical products in Japan, establishing a stable revenue foundation. This arrangement allows Chugai to concentrate its resources on unique and highly innovative technologies and drug discovery. Meanwhile, Chugai Pharmaceutical licenses out innovative drugs developed internally to Roche, which then supplies them to the global market. This enables Roche to sell pharmaceutical products innovated and developed by Chugai on a worldwide scale, thus creating a mutually beneficial relationship. In addition to having leading research in GLP-1 class peptide mimetics as small molecule agonists, Chugai Pharmaceutical also possesses a strong research foundation in KRAS and RAS class oral cyclic peptide inhibitors. Searching Chugai's latest patents in the Synapse database revealed an application opened on November 9, 2023, titled: ' Cyclic compound having inhibitory effect selective for kras but not for hras and nras'. The application was filed on May 2, 2023, and was made public just six months later. The patent document is very extensive, containing synthesis examples of more than 3,000 cyclic peptides and detailing the Kd values for KRAS, NRAS, HRAS, as well as the inhibitory IC50 values on NCI-1441 cells. The Kd value is calculated using Biacore, and the ratio of the Kd values of the other two subtypes to that of KRAS is denoted with letters. Ratios of Kd values greater than or equal to 0.1 and less than 3 are designated as C, ratios of 3 or higher and less than 10 are designated as B, ratios of 10 or higher and less than 20 are designated as A, and ratios of 20 or higher are designated as AA. The figure above lists two implementation examples, PP1087 and 1570, both of which are 12mer peptides with KRAS Kd values in the range of 0.05-0.09 nM, indicating a high affinity. Their selectivity is over 10-fold, although no compounds with over 20-fold selectivity have been observed yet. The cyclic peptides in this patent are notably different from Chugai Pharmaceutical's clinical cyclic peptide LUNA18, though both are 12mers. Additionally, the two exemplified implementations each have only three hydrogen bond donors (NH), and the large ring conformation exhibits flexibility, which can enhance gastrointestinal absorption of the drug to meet the bioavailability requirements for oral medications. In another patent by Chugai Pharmaceutical, WO2022234853, they disclosed their discovery of cyclic peptides and oligopeptide compounds that selectively inhibit KRAS. These peptidic compounds have been found to interact with specific amino acid residues of KRAS. The lead compound in this patent is PP-1501, with its selectivity determined through Kd values showing over 10-fold selectivity against HRAS and NRAS, and an IC50 value of 1.5 nM in inhibiting NCI-1441 cells. This is also a 12mer, containing three hydrogen bond donors and nine fluorine atoms within its molecule. This further illustrates that reducing the number of hydrogen bond donors/acceptors usually can improve the oral bioavailability of small molecules. Potentially reducing it further to below three might affect the activity and selectivity of this series of cyclic peptides, which is why Chugai Pharmaceutical consistently maintains three hydrogen bond donors in their cyclic peptides. In another pharmaceutical patent, WO2022234852, the inclusion of their clinical cyclic peptide molecule LUNA-18 is described. Aside from AsPC-1, LUNA-18 exhibited significant cytotoxic activity (IC50=0.17-2.9nM) against cell lines with KRAS gene mutations, such as LS180 (colorectal cancer, KRASG12D), GSU (gastric cancer, KRASG12D), NCI-H441 (non-small cell lung cancer, KRASG12V), NCI-H2122 (non-small cell lung cancer, KRASG12C), and MiaPaCa-2 (pancreatic cancer, KRASG12C). The in vivo efficacy of LUNA-18 was evaluated in NCI-H441 or MiaPaCa-2 xenograft models in mice. The compound LUNA-18 was administered orally once daily for a continuous period of 14 days, during which mouse body weight and tumor volume were measured. At a dose of 10 mg/kg, tumor regression was observed, with no significant weight loss noted. PK studies of luna18 were conducted in mice, rats, monkeys, and dogs. Following oral administration, the bioavailability of the compound luna18 in these four species ranged from 21% to 47%. On the 24th of last month, the Journal of the American Chemical Society (JACS) published the latest paper on the modification of a cyclic peptide inhibitor by Chinese and international pharmaceutical companies, in which the oral bioavailability of LUNA18 in various species was disclosed. In mice, a 10 mg/kg oral dose resulted in an exposure of 3600 ng*h/mL and a C_max of 780 ng/mL, indicating very good activity and an expectation to cover the concentration required for pharmacological efficacy. Rats showed slightly better performance compared to mice, with the C_max and AUC of IV and PO administration showing a doubling in growth, yet the bioavailability was only around 20%. Both dogs and monkeys exhibited longer half-lives, reaching 14 hours and 8 hours respectively, suggesting that the human oral half-life could also be over 10 hours and supporting once daily (QD) dosing in the clinic. Overall, mice, rats, dogs, and monkeys all showed low clearance, and improved absorption might further increase bioavailability (F). These results suggest that luna18, as an orally-administered cyclic peptide, holds therapeutic potential for treating various cancers carrying KRAS mutations. Currently, luna18 is in Phase 1 clinical trials in Japan and the USA. Due to the KRAS signaling pathway functioning through intracellular PPIs, usually involving large binding surfaces, medicinal chemists are also pursuing macrocyclic formats, including nucleic acids, peptides, antibodies, or non-immunoglobulin proteins. Cyclic peptides have attracted the attention of numerous companies. They are generally larger (500-3000 Da) than conventional small molecules, better suited to exploit the flat and hydrophobic interfaces characteristic of PPIs, and can exhibit antibody-like binding affinity and specificity with just a small fraction of their molecular weight. This is the theoretical basis for this class of macrocyclic peptide inhibitors to show high selectivity and fewer off-target side effects. Cyclic peptides also retain many desirable small molecule properties, such as low immunogenicity and resistance to proteolytic degradation. Chugai Pharmaceutical is undeniably a pioneer in the development of oral RAS and KRAS peptide inhibitors. After transferring a GLP-1 oral small molecule agonist (peptidomimetic) to Eli Lilly, they continue to make innovative strides in KRAS cyclic peptides using their peptide development platform, where each patent comprises several thousand embodiments, and each embodiment requires completion of over four biological tests. This craftsmanship is highly admirable and has yielded significant rewards. The content above comes from the network. if any infringement, please contact us to modify.

02 Mar 2025

·synapse.patsnap.com

Inventory of GPCR Targeted Drugs Applying for Listing (I)

This article will review currently applied listed GPCR-targeting drugs, and the associated popular GPCR class targets and drug development opportunities worth paying attention to. 1.Eli Lilly: Tirzepatide Target:GIPR + GLP-1R Tirzepatide is a novel GIPR and GLP-1R dual agonist developed by Eli Lilly. In preclinical and clinical trials, compared to selective GLP-1 receptor agonists, GIP/GLP-1 dual agonists have been shown to better control blood sugar and reduce weight. Therefore, it is receiving increasing attention as a new therapeutic drug for controlling blood sugar and weight. In 2022, Tirzepatide was approved for the first time in the United States for the treatment of adult type II diabetes as an adjunct to diet and exercise. Subsequently, Tirzepatide was approved in the European Union and Japan for the treatment of type II diabetes. 2.ChemoCentryx: Avacopan Target:C5aR Avacopan(Tavneos) is an orally administered, first-in-class selective complement 5a receptor (C5aR) antagonist, discovered and developed by ChemoCentryx. This drug is used as an adjunctive therapy for ANCA-associated vasculitis in adult patients. Anti-neutrophil cytoplasmic antibody-associated vasculitis (AAV) is a rare ("oligo-immune") systemic small-vessel vasculitis, with an estimated incidence of 3 per 100,000 annually, characterized by the presence of ANCAs in the serum. The entire course of AAV includes granulomatosis with polyangiitis (GPA), microscopic polyangiitis (MPA), eosinophilic granulomatosis with polyangiitis (EGPA), and drug-induced AAV. Despite its complex pathophysiology, research over the past approx. 20 years has determined the crucial role of the alternative complement pathway, particularly the interaction of C5a with the C5aR receptor in AAV. Avacopan was first approved for marketing in Japan on September 27, 2021, and was subsequently approved in the United States, European Union, Canada, and Australia for the treatment of adult patients with ANCA-associated vasculitis, granulomatosis with polyangiitis, and microscopic polyangiitis. In addition, research is ongoing for other potential clinical indications, such as hidradenitis suppurativa and C3 glomerulopathy. 3.Pfizer: Rimegepant Sulfate Target:CGRP Receptor Rimegepant is an orally administered CGRP receptor antagonist used for the acute treatment of migraine in adults, with or without aura. Initially developed by the BMS(BMS-742413), the newly established biotech company Biohaven Pharmaceutical acquired the exclusive global development and commercialization rights to Rimegepant in 2016. The Biohaven team conducted a series of clinical studies and analyses around Rimegepant and developed the derivative migraine nasal spray drug, Zavegepant. In May 2022, Pfizer announced that it would acquire Biohaven for a total cash consideration of approximately 11.6 billion USD. Rimegepant was first approved for marketing in the United States on February 27, 2020, and subsequently received approval in Israel, the United Arab Emirates, Kuwait, the European Union, and Iceland, among others. Currently, the drug is being tested in clinical trials for conditions like chronic sinusitis, nasal polyps, and trigeminal neuralgia. 4. Glenmark:RYALTRIS Target:H1R+GR RYALTRIS is a new compound prescription nasal spray developed by the Indian pharmaceutical company, Glenmark. This medication has the dual efficacy of activating glucocorticoid receptor (GR) and antagonizing histamine H1 receptor (H1R). Mometasone is a moderately potent synthetic corticosteroid that acts as a glucocorticoid receptor agonist, possessing anti-inflammatory, anti-itch, and vasoconstrictive properties. Olopatadine, on the other hand, is an antagonist of histamine H1 receptors used for the treatment of allergic conjunctivitis and rhinitis. Since histamine is the primary inflammatory mediator causing inflammation and allergic reactions, Olopatadine works by blocking the action of histamine receptors. Compared to other anti-allergic ophthalmic drugs, Olopatadine does not interfere with the cell membrane, thus offering good comfort and tolerability. RYALTRIS was first approved for marketing in Australia in 2019, and subsequently received approval for listing in South Africa, the UK, the US, Canada, and other countries. In 2019, Grand Pharmaceutical and Glenmark signed an exclusive licensing agreement, in which Glenmark granted Grand Pharmaceutical the exclusive rights to sell RYALTRIS in China. Glenmark would be responsible for the manufacture and supply of the authorized product, while Grand Pharmaceutical would be in charge of the clinical trials and registration work for the authorized product in China and can exclusively sell the approved product in China for 20 years upon approval. 5. Amgen:Erenumab Target:CGRP Erenumab is a human monoclonal antibody developed by Amgen and is the first monoclonal antibody drug targeting GPCR approved by the FDA. Erenumab can specifically bind to and antagonize the Calcitonin Gene-Related Peptide Receptor (CGRPR), thus preventing migraines. In April 2017, Amgen announced an expanded commercial collaboration with Novartis on Erenumab, which is being studied for the prevention of migraine. This expanded business cooperation is based on the global neuroscience collaboration established by Novartis and Amgen in 2015 in the areas of Alzheimer's disease and migraine. Novartis initiated two clinical trials in China in 2019 to evaluate the safety and efficacy of Erenumab injection in the treatment of migraines. Erenumab was first approved for marketing in the United States in 2018, and was subsequently approved in Australia, Iceland, Norway, Switzerland, Canada, and Japan. In addition to the treatment of migraines, clinical trial research is ongoing for other indications, including headaches, hot flashes, temporomandibular joint dysfunction syndrome, stable angina. 6. Kyowa Kirin:Evocalcet Target:CaSR Evocalcet is a Calcium-Sensing Receptor (CaSR) agonist developed by Kyowa Kirin, used for the treatment of hypercalcemia, secondary hyperparathyroidism, and other related conditions. Kyowa Kirin has applied for two clinical trials in China to evaluate the effectiveness of Evocalcet in treating secondary hyperparathyroidism in patients undergoing maintenance dialysis for chronic kidney disease. As of now, Evocalcet has only been approved for marketing in Japan. 7. Otsuka Pharmaceutical: Brexpiprazole Target:5-HT1A+5-HT2A+D2R Brexpiprazole is a serotonin-dopamine activity modulator developed by Otsuka Pharmaceutical, used as an adjunctive treatment for severe depression, schizophrenia, and agitation associated with dementia caused by Alzheimer's disease. Brexpiprazole is an atypical antipsychotic and a novel D2 dopamine and serotonin 1A partial agonist, known as a serotonin-dopamine activity modulator. It has a high affinity for serotonin, dopamine, and alpha-adrenergic receptors. Structurally, Brexpiprazole is very similar to another atypical antipsychotic drug, Aripiprazole, but Brexpiprazole has a different affinity for binding with dopamine and serotonin receptors. Compared to Aripiprazole, Brexpiprazole is less likely to produce adverse reactions mediated by partial agonist, such as extrapyramidal symptoms, due to its lower intrinsic activity at the D2 receptor. Brexpiprazole was first approved in the United States in 2015, and subsequently approved in Canada, Japan, and the European Union. In addition to treating depression, this drug is undergoing global clinical trials and research for multiple indications including agitation, schizophrenia, Alzheimer's disease, and performance anxiety. 8. Santen: Tapcom Target:PTGFR+βAR Tapcom is a combination eye drop medication containing Tafluprost and Timolol Maleate, developed by Santen. Tafluprost is a prostaglandin analogue used in ophthalmology to reduce intraocular pressure in patients with ocular hypertension or open-angle glaucoma. Chemically, Tafluprost is a fluorinated analogue of prostaglandin F2-α. Timolol is a non-selective beta-adrenergic antagonist, used for the treatment of elevated intraocular pressure in patients with ocular hypertension or open-angle glaucoma. Tapcom was first approved for marketing in Japan in 2013, and subsequently received approval in countries including Iceland, France, Poland, and Germany. 9. Takeda:TeduglutideTarget:GLP-2R Teduglutide is a glucagon-like peptide-2 (GLP-2) analog developed by the British rare disease pharmaceutical giant, Shire Development, for the treatment of patients with short bowel syndrome (SBS) who require parenteral nutrition support. Teduglutide is comprised of 33 amino acids, and is manufactured using strains of E. coli that have been modified through DNA recombinant technology. Teduglutide differs from GLP-2 by one amino acid (alanine is replaced with glycine). This substitution results in Teduglutide having a longer duration of action than endogenous GLP-2 and a higher resistance to hydrolysis by the enzyme dipeptidyl peptidase-4. Teduglutide first received regulatory approval within the European Union in 2012, followed by approval in the United States and Japan, in all cases for the treatment of SBS. In 2019, Takeda Pharmaceuticals spent an astounding £46 billion to acquire Shire Development, in a move that has been dubbed as a "snake swallowing an elephant" merger in the pharmaceutical world. This acquisition propelled Takeda Pharmaceuticals into the list of top 10 global biopharmaceutical companies. Clinical research on the application of Teduglutide for the treatment of Crohn's Disease and kidney disorders was discontinued due to this acquisition. 10. AstraZeneca: Duaklir GenuairTarget:M3R+β2AR Duaklir Genuair is a combined Aclidinium Bromide/Formoterol Fumarate inhalation powder developed by AstraZeneca. This medication is used as a maintenance bronchodilator to alleviate the symptoms of disease in adults with chronic obstructive pulmonary disease (COPD). Among them, Aclidinium bromide is a novel long-acting muscarinic antagonist, and Formoterol fumarate is a long-acting β2 receptor agonist. Duaklir Genuair is administered by the Genuair dry powder inhaler twice a day and is the first combined medication that has shown a statistically significant improvement over monotherapy in terms of shortness of breath. Duaklir Genuair was first approved in the European Union in 2012, and subsequently in the United States in 2019, for the treatment of chronic obstructive pulmonary disease. The content above comes from the network. if any infringement, please contact us to modify.

26 Feb 2025

·www.biopharmadive.com

Lilly expands US manufacturing build-out with $50B target

Eli Lilly will invest tens of billions more dollars in U.S. drug manufacturing in a significant enlargement of plans the Indianapolis company had already described as historic.Lilly, which makes the popular obesity medicine Zepbound, previously pledged to spend $23 billion on constructing and refurbishing factories in the U.S. to churn out the companys new pills and injections. On Tuesday, the company more than doubled that target. Including commitments made since 2020, it expects to pour over $50 billion into U.S. capital expenditures.According to Lilly, the planned spending is the largest pharmaceutical investment in domestic manufacturing of the past decade.The $27 billion in new investment will go toward building four drug production facilities, three of which will be dedicated to making the active pharmaceutical ingredients the industry regularly imports from abroad. Specifically, Lilly said its investment will help to reshore critical capabilities of small molecule chemical synthesis. The fourth site will support the companys global manufacturing network for injectable therapies.Overall, Lilly expects the four facilities will eventually employ more than 3,000 technicians, scientists and other personnel, as well as create nearly 10,000 construction jobs.Lilly announced its plans at a press conference in Washington, D.C., six days after company head David Ricks, along with his CEO peers at Pfizer and Merck & Co., met with President Donald Trump at the White House. According to Bloomberg, Trump warned the executives their industry could face tariffs if they dont move manufacturing back to the U.S. Earlier last week, Trump had said he would impose tariffs in the neighborhood of 25% on pharmaceuticals, among other goods.In a statement, Ricks said the companys decision to further invest in domestic manufacturing capacity reflected its conviction in its drug pipeline. But his statement included an economic message, too: Our confidence positions us to help reinvigorate domestic manufacturing, which will benefit hard-working American families and increase exports of medicines made in the U.S.A.Ricks also called for an extension of tax cuts passed in 2017 during Trumps first term, calling them foundational to Lillys domestic investment. In addition to lowering corporate levies,that law also reduced the rate at which profits earned overseas would be taxed upon repatriation to the U.S., aiding drugmakers in particular.Lilly, and the pharmaceutical industry more broadly, hope to secure similar benefits from this administration, as well as to revise a Biden-era lawthat for the first time allowed Medicare to directly negotiate drug prices. Earning Trumps support may be harder, however.Per Bloomberg, Trump didnt commit to making changes in his meeting with Ricks last week, and expressed dissatisfaction at the higher costs of drugs in the U.S. versus overseas.The commercial success of Zepbound has played a major role motivating Lillys manufacturing spending. The company initially struggled to keep up with demand, only recently resolving shortages that had opened the door for compounding pharmacies to make off-brand copies. Previously announced investments in Indiana and in Wisconsin were aimed at expanding production of Zepbound and drugs like it.Lilly hasnt yet finalized the locations for the four new factories. The company is currently in negotiations with several states and expects to announce the future site locations this year. It anticipates the new facilities will begin making drugs for patients within five years.Prior to 2022, Lilly averaged about $1.4 billion in annual capital expenditures. Spending increased to $3.45 billion in 2023 and $5.06 billion last year. Analysts expect Lilly sales, which reached $45 billion in 2025, to grow substantially on the back of Zepbound and successor obesity drugs the company is developing. '

100 Deals associated with Tirzepatide

External Link

KEGG	Wiki	ATC	Drug Bank
D11360	Tirzepatide	-	DB15171

R&D Status

Approved

10 top approved records.

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Indication	Country/Location	Organization	Date
Sleep Apnea, Obstructive	US	Eli Lilly & Co.	20 Dec 2024
Obesity	US	Eli Lilly & Co.	08 Nov 2023
Overweight	US	Eli Lilly & Co.	08 Nov 2023
Weight Gain	AU	Eli Lilly Australia Pty Ltd.	23 Dec 2022
Diabetes Mellitus, Type 2	US	Eli Lilly & Co.	13 May 2022

Developing

10 top R&D records.

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Indication	Highest Phase	Country/Location	Organization	Date
Heart failure with normal ejection fraction	NDA/BLA	CN	Eli Lilly & Co.	22 Nov 2024
Obesity Hypoventilation Syndrome	NDA/BLA	CN	Eli Lilly & Co.	15 Sep 2024
Plaque psoriasis	Phase 3	US	Eli Lilly & Co.	30 Sep 2024
Plaque psoriasis	Phase 3	PR	Eli Lilly & Co.	30 Sep 2024
Arthritis, Psoriatic	Phase 3	US	Eli Lilly & Co.	24 Sep 2024
Arthritis, Psoriatic	Phase 3	PR	Eli Lilly & Co.	24 Sep 2024
Cardiovascular Diseases	Phase 3	US	Lilly Asia Shanghai Representative Office	29 May 2020
Cardiovascular Diseases	Phase 3	US	Eli Lilly & Co.	29 May 2020
Cardiovascular Diseases	Phase 3	AR	Lilly Asia Shanghai Representative Office	29 May 2020
Cardiovascular Diseases	Phase 3	AR	Eli Lilly & Co.	29 May 2020

Clinical Result

Indication

Phase

Evaluation

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT03861052 (SURPASS J-mono, Pubmed \| Diabetes Ther)	Phase 3	Diabetes Mellitus, Type 2 C-peptide	636	Tirzepatide 5 mg	znhofqulfq(jeabmrbeei) = katdcqrygs khsekgxrlc (mhysfprusn ) View more	Positive	14 Feb 2025
				Tirzepatide 10 mg	znhofqulfq(jeabmrbeei) = nyericzloj khsekgxrlc (mhysfprusn ) View more
NCT04847557 (SUMMIT, Pubmed \| N Engl J Med)	Phase 3	Heart failure with normal ejection fraction	731	Tirzepatide	uctsgoiyaq(twpmcijtak) = mainly gastrointestinal, leading to discontinuation of the trial drug occurred in 23 patients (6.3%) in the tirzepatide group and in 5 patients (1.4%) in the placebo group skbpxyzffg (fqubyybfiq )	Positive	30 Jan 2025
				Placebo
NCT04166773 (SYNERGY-NASH, CTgov)	Phase 2	Nonalcoholic Steatohepatitis	190	Tirzepatide (5 mg Tirzepatide)	fqulooauks(lqrimapvaj) = vuhqmnabcj ongcunpypl (lxufwqcxoj, jjgixdvccx - xgzvcrkqkz) View more	-	24 Jan 2025
				Tirzepatide (10 mg Tirzepatide)	fqulooauks(lqrimapvaj) = msrmpviaoo ongcunpypl (lxufwqcxoj, evnvksvcoo - ivfeeafyfp) View more
Pubmed Manual	Not Applicable	Overweight \| Obesity	15,491	Tirzepatide 15 mg once weekly	ekzvliqacu(mhrendyfzj) = ffydzixyec shzhbaxiep (cuboicqqdp )	Positive	07 Jan 2025
				Semaglutide 2.4 mg once weekly	ekzvliqacu(mhrendyfzj) = pwuqhwncwc shzhbaxiep (cuboicqqdp )
NCT04093752 (SURPASSAP-Combo, NEWS) Manual	Phase 3	Diabetes Mellitus, Type 2	-	替尔泊肽 15mg每周一次	iyptjwnnzg(ueqtvgakpx) = zinlamhisi yxgtuhxvcc (difyavhatg ) View more	Positive	31 Dec 2024
NCT05822830 (SURMOUNT-5, Company_Website) Manual	Phase 3	Obesity	751	Zepbound (tirzepatide)	ahpbymagex(zsucewiqet) = jcdmjcvdue orugqemirn (xmjyunpjae ) View more	Superior	04 Dec 2024
				Wegovy (semaglutide)	ahpbymagex(zsucewiqet) = smnngiyssc orugqemirn (xmjyunpjae ) View more
NCT04847557 (SUMMIT, Pubmed) Manual	Phase 3	Heart failure with normal ejection fraction \| Obesity	731	Tirzepatide	lbwjsywtea(rwfvvctpxb) = seifwmqvbu dqmgpcyyri (awvokzzqnj ) View more	Positive	16 Nov 2024
				Placebo	lbwjsywtea(rwfvvctpxb) = xejwqxdfcj dqmgpcyyri (awvokzzqnj ) View more
NCT04184622 (SURMOUNT-1, Literature) Manual	Phase 3	Diabetes Mellitus \| Obesity	2,539	Tirzepatide	qitpcuqkab(yqbtpkgkuz) = qdainoyari demwxxrwcl (sbtkcratlk ) View more	Positive	13 Nov 2024
				Tirzepatide 5 mg	qitpcuqkab(yqbtpkgkuz) = wyyzmpznmh demwxxrwcl (sbtkcratlk ) View more
NCT04184622 (Pubmed \| N Engl J Med)	Phase 3	Diabetes Mellitus \| Obesity	-	Tirzepatide 5 mg	sqdorerbqf(ynqymaporn) = most common adverse events were gastrointestinal, most of which were mild to moderate in severity and occurred primarily during the dose-escalation period in the first 20 weeks of the trial nzdnwstixm (wkgoivuuql )	-	13 Nov 2024
				Tirzepatide 10 mg

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