This study is a 2-arm, double blinded, randomised clinical trial where 40 participants will be assigned 1:1 to insulin treatment alone (control) or insulin treatment and tirzepatide treatment for 32 weeks. The primary objective is to demonstrate that tirzepatide treatment, dose incremented to 15mg QW for 32 weeks adjunctive to insulin treatment can reduce body weight in patients with T1D and overweight or obesity when compared to insulin treatment alone. The secondary objective is to demonstrate that tirzepatide treatment, dose incremented to 15mg QW for 32 weeks can improve glycaemic control (measured by hbA1c), improve time in range, reduce insulin requirements, and reduce the severity of comorbidities in people with obesity and T1D. This trial includes a 6 month follow-up period.

Start Date01 Dec 2026

Sponsor / Collaborator

Royal North Shore Hospital

NCT07179120

/ Not yet recruitingPhase 2IIT

Male Fertility Preservation: Efficacy Evaluation of GLP-1Receptor Agonist Therapy for Infertility in Obese Males - A Multicenter Clinical Randomized Controlled Trial

Why is this study being done? Obesity can harm men's fertility by lowering sperm quality and hormone levels, making it harder to have children. Weight loss through diet and exercise helps, but it's often hard to stick with. New medicines called GLP-1 receptor agonists, like semaglutide (Ozempic) and tirzepatide (Mounjaro), help people lose weight and improve health. Early studies suggest these drugs might also boost sperm health in obese men, but more proof is needed. This study tests if these drugs can safely improve fertility in obese men who are having trouble conceiving.
What will happen in this study?
This is a 48-week study at several hospitals in China. About 180 men will be randomly assigned to one of three groups:
Group 1: Standard lifestyle changes, like a healthy diet and exercise, guided by experts.
Group 2: Weekly injections of semaglutide, starting low and increasing as tolerated.
Group 3: Weekly injections of tirzepatide, starting low and increasing as tolerated.
All men will have regular check-ups, including blood tests, semen analysis, and weight measurements. We will track sperm quality, hormone levels, weight loss, and whether their partners get pregnant naturally. The study includes an 8-week adjustment period, 24 weeks of treatment, and 16 weeks of follow-up.
Who can join this study? Men aged 20-45 who are married, obese (BMI 28 or higher or waist size 90 cm or more), and have been trying to have a baby for at least a year without success due to low sperm count or poor sperm movement. Their female partners must be under 40 and have no major fertility issues. Men must be willing to attend visits and provide samples. People with serious health problems, recent use of similar drugs, or other causes of infertility (like genetic issues) cannot join.
How long will this study last? The full study lasts 48 weeks (about 11 months), with visits every 4-8 weeks, plus monthly phone check-ins for pregnancy updates.
What are the possible benefits and risks? Benefits: If the drugs work, men may lose weight, improve sperm quality, and have a better chance of their partners getting pregnant naturally. They might also feel healthier overall. Risks: Common side effects include nausea, vomiting, or diarrhea from the drugs, which usually improve over time. Rare risks include pancreas inflammation or gallbladder issues. Lifestyle changes might cause minor injuries from exercise. All side effects will be monitored closely, and participants can quit anytime. Insurance covers any study-related harm.

Start Date01 May 2026

Sponsor / Collaborator

The First Affiliated Hospital of Wenzhou Medical College

NCT07191873

/ Not yet recruitingPhase 4IIT

A Phase IV Placebo-controlled Single Center Trial for Tirzepatide in Idiopathic Intracranial Hypertension Trial (TIIHT)

This will be a randomized, double-blind, parallel, placebo-controlled trial of 60 participants. The primary analysis will be a statistical comparison of the estimates of the mean difference in the 12-month change in intracranial pressure (ICP) between participants assigned to the tirzepatide and Placebo arms in 1:1 randomization using the intention-to-treat (ITT) population. Hypothesis testing will be performed using analysis of covariance (ANCOVA), with the treatment indicator as the independent variable and the 12-month change in ICP as the dependent variable. Models will include baseline ICP as a covariate. This primary endpoint will use a significance level of 0.05 to declare significance.

Start Date01 Feb 2026

Sponsor / Collaborator

Duke University

[+1]

100 Clinical Results associated with Tirzepatide

100 Translational Medicine associated with Tirzepatide

100 Patents (Medical) associated with Tirzepatide

1,314

Literatures (Medical) associated with Tirzepatide

01 Feb 2026·TISSUE & CELL

Tirzepatide enhances liver structural integrity by promoting mitochondrial dynamics and mitophagy via PINK1/PRKN and SIRT3/NRF2 pathways in an obese-diabetic-menopausal mouse model

Article

Author: Marinho, Thatiany S ; Aguila, Marcia B ; Marcondes-de-Castro, Ilitch A ; Mandarim-de-Lacerda, Carlos A

The effects on hepatic mitochondrial structure, mitophagy, and cellular homeostasis were investigated when treated with Tirzepatide (Tzp), a dual GIP/GLP-1 receptor agonist, in a mouse model combining obesity, type 2 diabetes, and menopause-conditions that collectively exacerbate metabolic dysfunction-associated steatotic liver disease (MASLD). Female C57BL/6 mice were fed either a control or high-fat, high-sucrose diet for 12 weeks, and half underwent bilateral ovariectomy to simulate menopause. Tzp was administered daily for four weeks. Liver tissue was evaluated for ultrastructural alterations, gene expression, and protein profiles. Untreated obese-diabetic and obese-diabetic-ovariectomized mice exhibited hepatocellular fat accumulation, mitochondrial swelling, and disorganized cristae, indicative of metabolic and oxidative stress. In contrast, Tzp-treated mice displayed preserved hepatic architecture and intact mitochondrial morphology. Tzp significantly downregulated autophagy genes (Ulk3, Atg5, Atg7) and key mitophagy regulators (PINK1, PRKN), reestablishing mitochondrial balance, primarily through the modulation of mitophagy and enhanced organelle stability. Simultaneously, it upregulated mitochondrial biogenesis markers (Ppargc1a, Tfam), antioxidant enzymes (SOD2, GR, GPX, CAT), and redox modulators (Sirt3, Nrf2), while normalizing oxidative stress-related genes (Nos1, Nox1). Tzp also mitigated endoplasmic reticulum (ER) stress by downregulating Atf4, Ddit3, and Gadd45 and rebalanced mitochondrial dynamics through the suppression of fission markers (Dnml1, Fis1) and the restoration of fusion mediators (Mfn1, Mfn2). Three-way ANOVA confirmed Tzp's broad regulatory effects on hepatic gene expression, while principal component analysis revealed clear transcriptional separation between treated and untreated groups. In conclusion, these findings demonstrate that Tzp preserves liver ultrastructure and restores mitochondrial dynamics, supporting its therapeutic potential in MASLD and hormone-related metabolic disorders.

01 Jan 2026·METABOLISM-CLINICAL AND EXPERIMENTAL

A melanocortin 4- and glucagon-like peptide 1 receptor multiple agonist for the treatment of diabetes and obesity

Article

Author: Roth, Christian L ; Chichura, Kylie S ; Doyle, Robert P ; den Hartigh, Laura J ; Ashlaw, Emily F ; Liu, Yongjun ; Mullins, Ginger ; Chepurny, Oleg G ; Holz, George G ; Elfers, Clinton T ; McGivney, Aelish ; Miranda, Isabella Chavez

Obesity and its sequelae cause significant morbidity and mortality worldwide. Current glucagon-like peptide-1 (GLP-1) receptor agonist-based treatments have significant side-effects associated with high rates of treatment discontinuation. Such concerns are greater still in children and adolescents. Thus, there remains a clinical unmet need to develop obesity and/or T2D mellitus therapies with significantly improved tolerability. Herein, we examined a polypharmacy approach combining melanocortin (MC) 4-, and GLP-1-receptor agonism in a single monomeric peptide based on α-MSH and Exendin-4 to bind and stimulate different peptide receptors in vitro, and to drive reductions in body weight and food intake in up to 7 weeks of treatment in comparison to semaglutide and tirzepatide as standard of care positive controls in diet-induced obese rats. Despite the monomeric peptide GLP-1-/MC4-receptor multiple agonist (KCEM1) being a non-lipidated, weaker GLP-1R agonist compared to semaglutide and tirzepatide, reductions in calorie intake and body weight were similar in all three groups after daily subcutaneous injections of the three peptides. In addition, KCEM1 offered superior glycemic control during glucose tolerance testing. In gene expression analyses, KCEM1, but not semaglutide or tirzepatide, significantly increased expression of glucose transporter 4 (GLUT4) and key glycolysis enzyme Pgk1 in skeletal muscle, while it reduced genetic markers of inflammation in different tissues, including inflammatory markers IL-6 and TNF-α in liver tissue. Furthermore, KCEM1 lowered hepatic lipid content and improved metabolic dysfunction-associated steatohepatitis (MASH) scoring. Overall, these data extend emerging concepts around the use of multi-receptor polypharmacy to treat metabolic syndrome.

01 Jan 2026·Methods in molecular biology (Clifton, N.J.)

Assessing the Role of PPKs in Phosphorylating Phytochrome A Using the Protoplast Transient Expression System

Article

Author: Feng, Ziyi ; Li, Jigang

Phytochrome A (phyA) is the far-red (FR) light photoreceptor in plants, and its phosphorylation status plays a critical role in modulating its protein activity and function. The protoplast transient expression system has become an increasingly efficient approach for analyzing promoter activities, protein subcellular localization, protein-protein interactions, etc. Recently, we employed the protoplast transient expression system to assess the role of the protein kinases PHOTOREGULATORY PROTEIN KINASES (PPKs) in phosphorylating phyA. TANDEM ZINC-FINGER/PLUS3 (TZP), a phyA-interacting protein previously shown to mediate phyA phosphorylation in vivo, was coexpressed with phyA and PPKs in Arabidopsis protoplasts. After the treatment with FR light, we observed that PPKs can directly phosphorylate phyA and that TZP enhances PPKs-mediated phosphorylation of phyA in Arabidopsis protoplasts. In this chapter, we will describe the detailed experimental procedures and the key points for implementing this system. This system may also be feasible for validating the relationship between other kinases and their potential substrates.

1,539

News (Medical) associated with Tirzepatide

26 Nov 2025

·pharma.economictimes.indiatimes.com

US Medicare price cuts manageable for most drugmakers, analysts say

London: U.S. Medicare price cuts of up to 85% will have a lesser impact on drugmakers than initially feared, with most of the hit already reflected in forecasts, Wall Street analysts said. Shares of Danish drugmaker Novo Nordisk and Teva Pharmaceuticals rose 5% and 3% respectively after the U.S. government published negotiated prices late on Tuesday. Novo's top-selling drug semaglutide, sold as Ozempic for diabetes and Wegovy for weight loss, as well as Teva's Austedo for Hungtington disease were among the closely watched drugs on the list of prices, which will take effect in 2027. The announcement and recent White House deals offer clarity on pricing for popular GLP-1 drugs such as Wegovy and Eli Lilly's Zepbound, which have drawn scrutiny over their costs. The negotiated price for Novo's semaglutide is "the final cloud to clear on the drawn-out, but positively resolved GLP-1 pricing debate ," said Bernstein analyst Christian Moore. The price cuts through the U.S. Medicare health plan come as President Donald Trump's administration pushes the drug industry to advocate for other wealthy nations, particularly in Europe, to pay more for prescription medicines. Goldman Sachs said a key question for the first half of 2026 will be whether lower Medicare prices boost Wegovy volumes. William Blair analysts noted the $274 monthly price for Novo's semaglutide broadly aligns with recent government deals, but said uncertainty remains over insurance coverage expansion. FACTORED INTO NOVO, ASTRAZENECA AND GSK FORECASTS Bernstein analysts said that five of the 15 targeted medicines will become generic by 2027, limiting their exposure to price cuts. The lower prices could even keep patients on the branded therapies longer, boosting volumes, they said. Analysts agreed that the reductions had been factored into estimates for Novo, AstraZeneca and GSK. Earlier this month, Novo said it expected a low single-digit impact to global sales if the price cuts were implemented this year. Analysts said that would imply roughly a 6 billion Danish crown ($931 million) sales hit. AstraZeneca and GSK shares were flat on Wednesday. GSK said when reporting third-quarter results that any impact from negotiated prices was fully factored into its outlook. Shore Capital analyst Sean Conroy said the cuts would hit earnings by "low- to mid-hundreds" of millions of pounds or dollars. Bernstein estimated the impact on Abbie in the range of $100 million to $250 million to sales of its mood disorder drug Vraylar and irritable bowel syndrome medicine Linzess as well as for Amgen's psoriasis drug Otezla. ($1 = 6.4404 Danish crowns) (Reporting by Bhanvi Satija and Maggie Fick in London, Stine Jacobsen in Copenhagen, Mariam Sunny and Mrinalika Roy in Bengaluru; Editing by Jane Merriman, Jan Harvey and Alexander Smith)

26 Nov 2025

·www.biospace.com

Novo’s GLP-1s Highlight List as CMS Unveils Final Prices For Second Cycle of Drug Negotiations

iStock, Zolak The discounts should be compared against the drugs’ “ultimate net price” rather than their indicated list price to gauge the true impact of the negotiations, BMO Capital Markets analysts said. Negotiations for the second cycle of the Inflation Reduction Act’s drug pricing program have wrapped up, and the Centers for Medicare and Medicaid Services on Tuesday released the final agreed-upon prices for the 15 covered medicines. The discounts from list prices negotiated by CMS range from 38% for Teva Pharmaceuticals’ Huntington’s disease chorea therapy Austedo to 85% for Merck’s diabetes drug Janumet. Novo Nordisk’s Ozempic and Wegovy—arguably the most closely-watched drugs on this list—will sustain a 71% cost cut from their list price. The prices are set to take effect on Jan. 1, 2027. Analyst responses to the list were subdued. The final negotiated prices, Guggenheim Partners wrote on Tuesday evening, turned out to be “roughly in line” with expectations. The firm pointed to “the extensive gross-to-net adjustments that the manufacturers are already providing on these drugs.” BMO Capital Markets, for its part, wrote in a note to investors, “We reiterate that the important comparison remains the difference between the product’s newly discounted price and the product’s ultimate net price, including rebates,” instead of their list prices. Guggenheim also pointed out that many of the drugs under negotiation have already peaked in sales or have biosimilar or generic competition expected soon. Therefore, “Any impact on sales from lower prices will only impact the companies for a handful of years.” The final maximum fair prices are listed below: Centers for Medicare & Medicaid Services Tuesday’s pricing reveal comes amid the Trump administration’s push to lower drug costs in the U.S., for which it has launched several initiatives and struck a number of deals. Earlier this month, for instance, the White House came to an agreement with Novo and fellow obesity leader Eli Lilly to offer their respective GLP-1 drugs through the government’s forthcoming direct-to-consumer (DTC) platform at a steep discount. Ozempic and Wegovy, which have list prices of $1,000 and $1,350 per month, respectively, will be available for $350 on TrumpRx, while Lilly’s Zepbound will drop from $1,068 per month to $346 on the DTC marketplace. When the oral versions of their obesity drugs hit the market, the pharmas also promised to make their initial doses available for $150. Aside from Novo and Lilly, other pharma companies have joined the TrumpRx program . Pfizer kicked off this trend in late September when it partnered with the government to offer some of its products—including the eczema drug Eucrisa and the migraine nasal spray Zavzpret—on the DTC site. AstraZeneca followed suit soon after and promised to put many of its inhalers on TrumpRx. The centerpiece of the administration’s pricing push is its Most Favored Nation rule , announced in May. This executive order directs drug costs in the U.S. to be lowered to the same level as they are in similarly developed nations—a pricing philosophy that guides the other government initiatives, including its DTC program.

25 Nov 2025

·pharma.economictimes.indiatimes.com

Undeterred by Novo Nordisk failure, scientists consider GLP-1s as Alzheimer's prevention

Chicago: Novo Nordisk 's highly anticipated but ultimately unsuccessful Alzheimer's trials were a long shot for the maker of blockbuster drugs Ozempic and Wegovy, but scientists are still asking if GLP-1 drugs should be tested to prevent the disease in people at risk. Novo's trials tested Rybelsus , an older pill form of semaglutide, the same main ingredient in Ozempic and Wegovy injections. The drug failed to meet the studies' primary goal of delaying cognitive decline in hundreds of people with early-stage Alzheimer's disease. But in a release scant on details, the Danish drugmaker said Rybelsus did improve some unspecified Alzheimer's-related biological processes in both trials - clues that could help guide new studies, Alzheimer's experts said. That leaves open "a tiny window of hope that in future this drug might be effective if used earlier as a preventative strategy," said Professor Tara Spires-Jones, director of the Centre for Discovery Brain Sciences at the University of Edinburgh. Spires-Jones noted that diabetes and obesity are both associated with increased risk of developing Alzheimer's, conditions that are treated effectively with the GLP-1 drugs now taken by millions of people. "Future trials are needed to confirm whether GLP-1 drugs might be effective in preventing Alzheimer's disease," she said. Other GLP-1 drugs include Novo rival Eli Lilly's Zepbound and Mounjaro, which also hit an additional target called GIP. DETAILS EXPECTED NEXT WEEK Novo plans to discuss the findings at an Alzheimer's conference in San Diego on December 3. Dr. Eric Reiman, chief executive of the Banner Alzheimer's Institutes in Arizona, said the results are disappointing but do not rule out GLP-1s for people at risk of the disease but who don't yet have symptoms. "I'm eager to see the trials' biomarker findings and other details of the study next week, including any findings that might help the field consider its potential benefits in cognitively unimpaired people," he said. Dr. Zaldy Tan, a geriatrician at Cedars-Sinai in Los Angeles, said Novo's cancellation of the one-year follow-up trial suggested to him that "it wasn't promising at all." Nevertheless, he said he is waiting to hear about other outcome measures, such as changes in Alzheimer's-related proteins in the blood. DATA SHOW EARLY GLP-1s CUT DEMENTIA RISK Novo's trials focused on people with early Alzheimer's disease as confirmed by the presence of clumps of a protein called beta amyloid in their brain, the target of the two approved treatments for the mind-wasting condition. Much of the evidence from large population studies suggesting a potential benefit from GLP-1s comes from studies of people with diabetes who are at increased risk of vascular dementia, a condition marked by damage in small blood vessels in the brain. An April study in JAMA Neurology of medical records from nearly 400,000 people with diabetes aged 50 and older found that those taking GLP-1s had a 33% reduced risk of developing dementia. "When we look back at very large populations, people who got GLP-1s appeared to not get Alzheimer's disease as frequently as people who did not take it or who took different diabetes medications," said Dr. Steven DeKosky of the University of Florida's Alzheimer's Disease Research Center in Gainesville, who was part of that study team. Even before Novo's preliminary results were released, Dr. Mary Sano, a Mount Sinai Alzheimer's researcher and an investigator in the trials, expressed concern that the focus on testing the drug in patients with confirmed Alzheimer's may have inadvertently excluded many people with diabetes and potentially vascular dementia from the trial. Ivan Koychev, clinical associate professor in neuropsychiatry at Imperial College London, said in an emailed comment that when the disease is more advanced, preventing further decline in the underlying biology may not be sufficient to show a clinically meaningful benefit. "This is a recurring theme in Alzheimer's disease therapeutics," he wrote. "The results reinforce the need to test these agents much earlier, ideally years before symptoms emerge, when neuronal systems are more intact and the potential for clinical benefit is greater." (Reporting by Julie Steenhuysen; Editing by Caroline Humer and Bill Berkrot)

Clinical ResultClinical Study

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	Czechia	Eli Lilly & Co.	26 Jun 2025
Colitis, Ulcerative	Phase 3	Denmark	Eli Lilly & Co.	26 Jun 2025
Colitis, Ulcerative	Phase 3	France	Eli Lilly & Co.	26 Jun 2025

Clinical Result

Indication

Phase

Evaluation

View All Results

Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT05822830 (SURMOUNT-5, CTgov)	Phase 3	Obesity	751	Tirzepatide (15 mg or MTD - Tirzepatide)	rromjfzetl(jrcronblgc) = hpoghycwlw wybxvmrjia (sqdukcbmdb, 0.59) View more	-	26 Nov 2025
				Semaglutide (2.4 mg or MTD - Semaglutide)	rromjfzetl(jrcronblgc) = golxzrtzdu wybxvmrjia (sqdukcbmdb, 0.59) View more
NCT04657016 \| NCT04660643 \| NCT04184622 (SURMOUNT-1, Pubmed \| Obesity (Silver Spring))	Phase 3	Obesity	2,788	Tirzepatide	ilqzinwurb(ougxxjrkxv) = ccluzztlcq gplyihbwmp (grlgzwybmx ) View more	Positive	04 Nov 2025
NCT04657003 \| NCT05536804 \| NCT04184622 (SURMOUNT-1, Pubmed \| J Am Soc Nephrol)	Not Applicable	-	3,477	Tirzepatide	yskaconjlp(apewkdxpdl): Difference (%) = −55.2 (95.0% CI, −68.5 - −36.4) View more	Positive	01 Nov 2025
				Placebo
ACR2025	Not Applicable	Overweight \| Obesity	62,722	Tirzepatide	opydmbsrbj(txpvfisiau): HR = 0.88 (95.0% CI, 0.81 - 0.95) View more	Positive	24 Oct 2025
				Phentermine
NCT05963022 (CTgov)	Phase 3	Diabetes Mellitus, Type 2	206	Tirzepatide (10 mg Tirzepatide)	rvabtipwdd(wtxxvszzyn) = lfuvszbfhv rqcubsqbhg (qyffogmaaq, 0.131) View more	-	21 Oct 2025
				Tirzepatide (15 mg Tirzepatide)	rvabtipwdd(wtxxvszzyn) = uqgudkfduv rqcubsqbhg (qyffogmaaq, 0.124) View more
NCT06914141 \| NCT06914154 \| NCT06914102 (Pubmed \| JAMA)	Not Applicable	Heart failure with normal ejection fraction	97,790	Semaglutide	lqxqfcqgkf(kgdksifmsc): HR = 0.58 (95.0% CI, 0.51 - 0.65) View more	Positive	14 Oct 2025
				Tirzepatide
NCT05260021 (SURPASS-PEDS, PRNewswire) Manual	Phase 3	Diabetes Mellitus, Type 2	99	Mounjaro 5 mg	fsfcyzpnwx(deytwwoohg) = rgkmlbxgly mweovtsjwl (qvxylmajex ) Met View more	Positive	17 Sep 2025
				Mounjaro 10 mg	fsfcyzpnwx(deytwwoohg) = mfgudilibp mweovtsjwl (qvxylmajex ) Met View more
NCT05412004 (SURMOUNT-OSA, WSC2025 \| ATS2025)	Phase 3	Sleep Apnea, Obstructive	623	Tirzepatide	tfdlkhksot(pnrtihippo): P-Value = 0.032 View more	Positive	05 Sep 2025
				Placebo
NCT05822830 (SURMOUNT-5, NEWS) Manual	Phase 3	Obesity	-	Tirzepatide	teswsaqpte(wdthmadnkv) = bywfstxwza yaykexhchh (onkiizaomg ) View more	Positive	01 Sep 2025
				Semaglutide	teswsaqpte(wdthmadnkv) = ykfmbbmgmu yaykexhchh (onkiizaomg ) View more
NCT04311411 (Pubmed \| Nat Med)	Phase 1	Overweight \| Obesity	114	Tirzepatide	argitvrcdp(miohdefdum) = grvvhcxtln uljyzhgwjp (nmtjkjssfg, -648.1 to -401.0)	Positive	01 Sep 2025
				Placebo	-

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