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

National Institute on Drug Abuse

NCT06801015

/ Not yet recruitingPhase 4IIT

A Randomized, Placebo-Controlled Trial of the Effects of Long-Acting GLP-1 or Dual Incretin (GLP-1 and GIP) Modulation on Gastric Motor Functions

The purpose of this study is to compare effects of weekly SQ semaglutide 2.4mg SQ, SQ tirzepatide 10mg, and placebo administered for 24 weeks on GES measured repeatedly at baseline, 16 weeks, 24 weeks, 28 weeks, 4 weeks after stopping the medication, and accommodation and satiation at 24 weeks compared to baseline.

Start Date15 Aug 2025

Sponsor / Collaborator

Mayo Clinic

100 Clinical Results associated with Tirzepatide

100 Translational Medicine associated with Tirzepatide

100 Patents (Medical) associated with Tirzepatide

1,232

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 Dec 2025·Current heart failure reports

Therapeutic Potential of GLP-1 Receptor Agonists in Heart Failure with Preserved Ejection Fraction (HFpEF) in Obese Patients

Review

Author: Patel, Ravi ; Ukah, Joan Dumebi ; Adejumo, Faith Adedayo ; Olatunji, Gbolahan ; Babalola, Adetola Emmanuel ; Ndakotsu, Andrew ; Kokori, Emmanuel ; Aderinto, Nicholas ; Abraham, Israel Charles

PURPOSE OF REVIEW:

Heart failure with preserved ejection fraction (HFpEF) is increasingly prevalent among individuals with obesity, primarily due to metabolic dysfunction and structural cardiac remodeling. This review explores the emerging therapeutic role of glucagon-like peptide-1 receptor agonists (GLP-1 RAs) in managing HFpEF in obese populations.

RECENT FINDINGS:

Recent clinical trials, including the STEP-HFpEF and SUMMIT studies, have shown that GLP-1 RAs such as semaglutide and tirzepatide significantly reduce body weight (13.3% and 13.9%, respectively), enhance exercise capacity (increases of 21.5m and 26m in 6-minute walk distance), and improve quality of life (19.5 and 16.6-point increases in KCCQ-CSS scores). Additionally, both agents demonstrated marked reductions in systemic inflammation, with C-reactive protein levels decreasing by 38.8% and 43.5%, respectively. GLP-1 RAs represent a promising class of agents targeting the cardiometabolic axis in HFpEF, offering meaningful improvements in functional capacity and symptom burden among obese patients. However, current evidence is limited by short trial durations, lack of population diversity, and insufficient long-term data. Future research should focus on more inclusive cohorts and extended outcomes such as hospitalization rates and cardiovascular events to fully define the long-term safety and efficacy of GLP-1 RAs in HFpEF management.

01 Nov 2025·DIAGNOSTIC MICROBIOLOGY AND INFECTIOUS DISEASE

In-vitro activity of cefepime/enmetazobactam against extended spectrum beta-lactamases and/or ampC producing Enterobacterales and Pseudomonas aeruginosa collected across India

Article

Author: Rodrigues, Camilla ; Shankar, Abirami ; Karthik, Rajiv ; Soman, Rajeev ; Veeraraghavan, Balaji ; Dwarakanathan, Hariharan ; Abdullah, Fiza ; Ramasubramanian, V ; KrishnaMoorthy, Soniya ; Nambi, Senthur ; Raj, Santhosh ; Manesh, Abi ; Srinivasan, Devishree ; Solaimalai, Dhanalakshmi ; Deswal, Vikas ; Nagvekar, Vasanth ; Ragothaman, Harathi ; Bakthavatchalam, Yamuna Devi ; Manokaran, Yuvasri ; Kumar, Deepak ; Varghese, George M ; Todi, Subash

BACKGROUND:

Extended spectrum beta-lactamase producing Enterobacterales are classified as critical priority pathogens with limited therapeutic options. Enmetazobactam is a novel penicillanic sulfone beta-lactamase inhibitor with the spectrum of coverage against range of ESBLs. The combination of cefepime/enmetazobactam has been approved for the treatment of cUTI including acute pyelonephritis in United States and Europe, and additionally licensed for the treatment of hospital acquired pneumonia including ventilator associated pneumonia and their associated bacteremia in Europe. In this study, we determined the in-vitro activity of cefepime/enmetazobactam along with comparators against molecularly well characterised third generation cephalosporin resistant Enterobacterales and P. aeruginosa isolates METHODS: Non-duplicate third generation cephalosporin resistant Enterobacterales (E. coli, n = 262; K. pneumoniae, n = 250; Enterobacter sp., n = 32; Proteus spp., n = 22) and P. aeruginosa (n = 100) clinical isolates were included in this study. Presence of ESBLs, ampCs and OXA-1 encoding genes were detected by PCR. MICs of cefepime/enmetazobactam and comparators were determined by reference broth microdilution. Time kill assay was performed to assess the antibacterial activity of cefepime/enmetazobactam against ESBL and/or ampC producers.

RESULTS:

Cefepime/enmetazobactam potently inhibited all CTX-M and/or OXA-1 producing E. coli isolates at MIC of ≤ 2 mg/L and ampC (CMY and/or DHA) producing isolates at MIC of ≤ 4 mg/L. Among CTX-M producing E. coli, susceptibility to TZP was significantly dropped from 78% to 58% in the presence of OXA-1. Further, cefepime/enmetazobactam continued to show potent activity against CTX-M producing K. pneumoniae and were inhibited at MIC of ≤ 1 mg/L. All the tested P. aeruginosa isolates were highly susceptible to cefepime/enmetazobactam with 100% inhibition. In time-kill assay, cefepime/enmetazobactam showed ≥ 3 log₁₀ kill against CTX-M producingE. coli and CTX-M producingK. pneumoniae isolates, which is comparable to that of meropenem.

CONCLUSION:

The findings of the present study retraites that the spectrum of coverage of cefepime/enmetazobactam is superior to that of TZP and similar to that of meropenem, emphasising the importance of cefepime/enmetazobactam as a carbapenem-sparing option.

1,360

News (Medical) associated with Tirzepatide

23 Jul 2025

·www.fiercebiotech.com

Apnimed\'s sleep apnea asset goes 2 for 2 in phase 3, solidifying star potential

If approved, Apnimed\'s AD109 would provide a far less cumbersome treatment for sleep apnea, which is most often addressed by wearing a mask hooked up to a CPAP machine while sleeping. \n Apnimed has scored another phase 3 knockout. The Massachusetts biotech’s daily pill for obstructive sleep apnea (OSA) reduced the number of nightly breath-stopping events by 46.8%, smashing the primary endpoint of the randomized, placebo-controlled, double-blind LunAIRo study and setting up the company for a new drug application submission by early 2026.Patients in the placebo arm scored just a 6.8% drop in OSA severity as assessed by the apnea-hypopnea index (AHI), a measure of the average number of times a patient either stops breathing or experiences shallow breathing per hour while sleeping, Apnimed announced in a July 23 release.The company also reported that there were no serious adverse events related to the treatment, called AD109, and that all treatment-related adverse events were mild or moderate. LunAIRo enrolled 660 adult patients from across the U.S.Though treatment lasted for a year, with the trial wrapping up in May, AHI scores for the primary endpoint were taken at the 26-week mark. The statistically significant drop in disease severity compared to placebo persisted to the end of the treatment period, Apnimed said.The LunAIRo results come two months after Apnimed dropped top-line results from another pivotal phase 3 trial called SynAIRgy. That trial was similar to LunAIRo, enrolling 646 participants and testing their AHI scores after six months of nightly AD109 doses. SynAIRgy found a similarly significant drop in AHI of 55.6%. “With two large phase 3 studies now demonstrating a consistent and significant efficacy profile for AD109, we are closer to delivering the first oral pharmacotherapy for over 80 million U.S. adults with OSA,” Apnimed CEO Larry Miller, M.D., said in the release. “We believe AD109, as a simple once-daily oral drug, has the potential to expand and reshape the treatment landscape.”Apnimed also shared a selection of other results from LunAIRo, including that AD109 significantly improved oxygenation and that 22.5% of patients receiving the asset had their OSA completely controlled at the end of the trial, defined as an AHI score lower than five.AD109 is a combination of aroxybutynin, a novel antimuscarinic, and atomoxetine, a noradrenaline reuptake inhibitor that is also used in attention-deficit/hyperactivity disorder. The compound targets the motor neurons that control breathing during sleep and boosts their activity so that throat muscles don’t relax, which is what causes breathing disruptions in patients with OSA.If approved, AD109 would provide a far less cumbersome treatment for OSA, which is most often addressed by wearing a mask hooked up to a CPAP machine while sleeping. This device pumps air into the airway so that pressure doesn’t drop low enough for muscles to collapse.Apnimed is already preparing for AD109’s commercial launch, tapping Pfizer veteran Graham Goodrich as chief commercial officer in January 2024.Should it secure the FDA’s green light, AD109 would be the first prescription drug designed specifically for sleep apnea. Eli Lilly’s weight loss drug Zepbound (tirzepatide) became the first ever FDA-approved sleep apnea med in December 2024 but is only approved for adults with obesity.

Clinical ResultPhase 3Drug Approval

23 Jul 2025

·www.biospace.com

GLP-1s Could Protect Against Neurodegeneration, Study Finds

iStock, BeritK A retrospective cohort study found that semaglutide and tirzepatide are linked with significantly lower risks of dementia and stroke, hinting at potential neuroprotective effects of GLP-1 therapies. Novo Nordisk’s semaglutide and Eli Lilly’s tirzepatide—both leading GLP-1 agonists used for weight loss and diabetes—are associated with a lowered likelihood of developing neurodegenerative disorders such as dementia, according to a recent study. The retrospective cohort study, published last week in JAMA Network Open , looked at electronic health record data of more than 60,800 adults 40 years and above with type 2 diabetes and obesity who had initiated treatment with semaglutide, tirzepatide or other antidiabetic drugs. Patients with prior neurodegenerative or cerebrovascular conditions were excluded from the analysis. Over seven years of follow-up, patients treated with GLP-1 analogs were 37% less likely to develop dementia than counterparts on other antidiabetic medications. This effect was statistically significant. Aside from dementia, the risks of ischemic stroke and all-cause mortality were likewise significantly reduced in patients treated with GLP-1s, with effect sizes of 19% and 30%, respectively. In contrast, GLP-1 therapies were not associated with altered risk of Parkinson’s disease, mild cognitive impairment and intracerebral hemorrhage versus other antidiabetic agents. These findings carry the usual caveats of a cohort study, namely that it could carry “residual confounding from unmeasured factors,” according to the paper’s authors, such as the patients’ functional status and frailty. The database that the study drew from also does not have biomarker and genetic data or neuroimaging information, leaving a mechanistic blind spot for its results. Still, these findings point to the “potential neuroprotective and cerebrovascular benefits” of GLP-1 drugs, according to the researchers, who added that future randomized trials in these patient populations are needed to “validate our findings and establish causality.” Novo is already working toward that end. The Danish pharma is running the Phase III EVOKE and EVOKE Plus studies to test semaglutide in Alzheimer’s disease. Both studies have a primary completion date in September 2025. Novo has also previously tested its older-generation GLP-1 therapy liraglutide in a Phase IIb study and found that treated patients saw 18% slower cognitive decline than those on placebo. For Lilly, the neuroprotective effects of tirzepatide could make the obesity drug a good complement to Kisunla, an anti-amyloid antibody approved in July 2024 for Alzheimer’s disease. The pharma is currently running the Phase III TRAILBLAZER ALZ-3 trial to test Kisunla in patients with preclinical disease. In a July 22 note to investors, analysts at BMO Capital Markets said that the trial could read out sooner than expected, “potentially by the start of 4Q25.” Additionally, even an interim analysis could be sufficient to detect statistical significance on disease progression. In such a case, analysts added, data from TRAILBLAZER ALZ-3 “could illustrate the value of treating presymptomatic patients with beta-amyloid therapies.”

Phase 2Phase 3Drug ApprovalClinical Result

17 Jul 2025

·www.biopharmadive.com

Bristol Myers, Pfizer to offer Eliquis at a discount for some patients

Bristol Myers Squibb and Pfizer will begin offering their top-selling heart medicine Eliquis through a new online service at a discounted price the latest example of pharmaceutical companies establishing direct-to-consumer options to bypass traditional drug distribution channels.The two companies, which sell the blood-thinning drug through a longstanding joint venture, said Thursday that theyll offer it at a discount of over 40%to people who are uninsured, underinsured or pay for the medicine out of pocket. The service distributing the medication, Eliquis 360 Support, will begin making shipments to U.S. patients on Sept. 8.A 30-day supply of Eliquis currently has a list price of $606, but would cost $346 per month under the new program, according to a report from the Wall Street Journal.Since its approval in 2012, Eliquis has been one of the worlds best-selling drugs, used to reduce the risk of clots and strokes in people with a variety of heart problems. Combined worldwide sales for Bristol Myers and Pfizer surpassed $20 billion last year.Settlement deals have also delayed the entry of generic competitors, keeping its list price high until at least 2026, when key patents in the U.S. and Europe are set to expire.The drugs profile made it a target of the federal government under the Biden administration, which, through the Inflation Reduction Act, bestowed Medicare the authority to negotiate prices for some prescription medications. As a result of those talks, Eliquis Medicare list price will be cut to $231 lower than the companies newly offered discount next year. The Journal reported that Thursdays announcement was driven by more government pressure, this time from the Trump administration, which has made drug prices a target and, through an executive order, called on the industry to offer medicines directly to patients at lower costs. However, most people in the U.S. access drugs through commercial or government-backed health plans, limiting the likely reach of these direct-to-consumer programs to people willing to pay cash or without insurance. Nonetheless, direct-to-consumer distribution channels, which sidestep insurers and pharmacy benefit managers, have been gaining momentum over the last year or so. Eli Lilly and Novo Nordisk have established online services for their obesity drugs Zepbound and Wegovy, and Pfizer last year set up a way to access savings programs for its migraine, COVID-19 and influenza medicines.This movement is different from what it was in the past, as pharmaceutical companies are setting these channels earlier in a drugs life cycle, rather than using them as tools to compete with lower-cost generics. '

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
Obesity Hypoventilation Syndrome	China	Eli Lilly Suzhou Pharmaceutical Co. Ltd.	30 Jun 2025
Sleep Apnea, Obstructive	United States	Eli Lilly & Co.	20 Dec 2024
Obesity	United States	Eli Lilly & Co.	08 Nov 2023
Overweight	United States	Eli Lilly & Co.	08 Nov 2023
Weight Gain	Australia	Eli Lilly Australia Pty Ltd.	23 Dec 2022
Diabetes Mellitus, Type 2	United States	Eli Lilly & Co.	13 May 2022

Developing

10 top R&D records.

to view more data

Indication	Highest Phase	Country/Location	Organization	Date
Heart failure with normal ejection fraction	NDA/BLA	China	Eli Lilly & Co.	22 Nov 2024
Colitis, Ulcerative	Phase 3	United States	Eli Lilly & Co.	26 Jun 2025
Colitis, Ulcerative	Phase 3	Austria	Eli Lilly & Co.	26 Jun 2025
Colitis, Ulcerative	Phase 3	Belgium	Eli Lilly & Co.	26 Jun 2025
Colitis, Ulcerative	Phase 3	Brazil	Eli Lilly & Co.	26 Jun 2025
Colitis, Ulcerative	Phase 3	Bulgaria	Eli Lilly & Co.	26 Jun 2025
Colitis, Ulcerative	Phase 3	Canada	Eli Lilly & Co.	26 Jun 2025
Colitis, Ulcerative	Phase 3	Croatia	Eli Lilly & Co.	26 Jun 2025
Colitis, Ulcerative	Phase 3	Czechia	Eli Lilly & Co.	26 Jun 2025
Colitis, Ulcerative	Phase 3	Denmark	Eli Lilly & Co.	26 Jun 2025

Clinical Result

Indication

Phase

Evaluation

View All Results

Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT04184622 (SURMOUNT-1, Pubmed \| Ann Intern Med)	Phase 3	Obesity	1,605	Tirzepatide 5 mg	gukrmcpvzf(pyurfyvkoe) = nummjiwxgm povndqfaxc (sebzlqezdu, -63.6% - -55.3%) View more	Positive	24 Jun 2025
NCT04311411 (Pubmed \| Nat Med)	Phase 1	Overweight \| Obesity	114	Tirzepatide	nbkqgluwip(rgphkpvaiy) = hkptgdmynd toxuaooiqk (uqvgbfwfer, -648.1 to -401.0)	Positive	24 Jun 2025
				Placebo	-
NEWS Manual	Not Applicable	Obesity	-	Semaglutide/Tirzepatide	aisuehsmeg(wyfdukzzqk) = ksudgzciut ccazdmpbqn (fhvrtmgflm ) View more	-	10 Jun 2025
ASCO2025	Not Applicable	Neoplasms	-	Tirzepatide	kkbzfrfeqg(ewqxoanlim) = rfhezekdqe jkphwyyqmr (zfxgzhtuvp )	Positive	30 May 2025
				GLP-1 receptor agonists	kkbzfrfeqg(ewqxoanlim) = gwxwvalfuh jkphwyyqmr (zfxgzhtuvp )
ATS2025	Not Applicable	Pulmonary Disease, Chronic Obstructive	-	GIP/GLP-1 co-agonist	tshwobzali(skgoqszhif): HR = 1.03 (95% CI, 0.88 - 1.21) View more	Positive	16 May 2025
				GLP-1 agonist
ATS2025	Not Applicable	Hyponatremia	-	Tirzepatide	tprwbifqtb(ghucauxrfn) = AKI (creatinine 2.38) mtphjxpxtt (kduwmzsolo ) View more	Negative	16 May 2025
				IV 0.9% sodium chloride
SURMOUNT-OSA (ATS2025)	Phase 3	Sleep Apnea, Obstructive triglycerides \| HDL-C \| non-HDL-C ... View more	-	Tirzepatide 10 mg	mxphuelehy(ommzclyjge) = eydvzxtgnc rjyeozulvl (zmmrminwgo ) View more	Positive	16 May 2025
				Tirzepatide 15 mg	mxphuelehy(ommzclyjge) = uofomlksxx rjyeozulvl (zmmrminwgo ) View more
ATS2025	Not Applicable	Idiopathic Pulmonary Fibrosis	-	GLP-1 agonists	wxhqvmmwry(ktwouteffc): HR = 0.62 (95% CI, 0.53 - 0.74), P-Value = <0.01	Positive	16 May 2025
				Glucagon-Like Peptide-1 Agonists (No GLP-1 agonists)
NCT05564039 (SURPASS-SWITCH, Pubmed \| Ann Intern Med)	Phase 4	Diabetes Mellitus, Type 2	282	Tirzepatide	hynlxfslee(xkeioobbpg) = ucxuhnpujf fnwhnwyetg (guodomylsf, 0.07) View more	Positive	01 May 2025
				Dulaglutide	hynlxfslee(xkeioobbpg) = jcjwohuyil fnwhnwyetg (guodomylsf, 0.08) View more
NCT05412004 (SURMOUNT-OSA, CTgov)	Phase 3	Sleep Apnea, Obstructive \| Obesity	469	Tirzepatide (Tirzepatide MTD_GPI1)	yyisvwrcqm(grjourrxei) = psogzcbrin yvureeunnn (codqaffyiq, 2.06) View more	-	30 Apr 2025
				Placebo (Placebo_GPI1)	yyisvwrcqm(grjourrxei) = yyogytrvzs yvureeunnn (codqaffyiq, 2.11) View more

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