Name: Retatrutide 10mg vial
Brand: Mijn winkel
SKU: 10
Price: 65.00 EUR
Availability: InStock

Vial labeled 'Retatrutide 10 mg' with batch number and expiration date on a neutral background

1/2

Retatrutide 10mg vial

€65,00 EUR

세금이 포함된 가격입니다.

NOT FOR HUMAN CONSUMPTION

Retatrutide is a once-weekly, acylated triple-agonist peptide that activates GLP-1, GIP, and glucagon receptors. The GLP-1/GIP components drive appetite suppression, insulinotropic effects, and β-cell support, while the glucagoncomponent adds energy-expenditure and fat-oxidation signals and may improve hepatic steatosis. In early–mid-stage trials, the tri-agonist profile has produced exceptional weight loss and metabolic improvements. Retatrutide is investigational (not FDA/EMA-approved).

Additional Benefits of Retatrutide Now Under Investigation

Benefit	Key take-aways
1 Unprecedented weight loss	Phase 2 obesity cohorts reported ~20–25% mean body-weight reduction at 48 weeks on higher doses, with curves still trending down—exceeding typical GLP-1 and even dual GIP/GLP-1 results. <br/><em>New England Journal of Medicine</em>
2 Potent glycaemic control	In type 2 diabetes, A1c reductions approaching ~2% with parallel fasting-glucose and post-prandial improvements; many participants reach A1c <7% without rescue therapy. <br/><em>JCEM; Diabetes Care</em>
3 Liver-fat & MASH signals	Marked MRI-PDFF decreases and ALT/AST improvements suggest meaningful NAFLD/MASHactivity, consistent with glucagon-mediated hepatic lipid mobilization plus weight loss. <br/><em>Hepatology; Liver International</em>
4 Cardiometabolic risk profile	Triglycerides fall, HDL rises modestly, and non-HDL/apoB trend down; blood pressure often drops ~6–10/3–5 mmHg with waist-circumference shrinkage. <br/><em>Circulation; Atherosclerosis</em>
5 Higher energy expenditure	Human calorimetry and preclinical data show ↑ resting energy expenditure and fat oxidation, attributed to glucagon receptor activation—countering adaptive metabolic slowdown. <br/><em>Cell Metabolism; Nature Metabolism</em>
6 OSA & mobility	Large weight loss translates to improved AHI (sleep apnea) and better functional capacity/painmarkers in obesity substudies. <br/><em>Chest; Obesity</em>
7 Early β-cell/insulin-sparing effects	GIP/GLP-1 synergy improves first-phase insulin and glucose-dependent control, allowing de-intensification of other diabetes meds in some participants. <br/><em>Diabetes; Diabetologia</em>
8 Visceral-fat and ectopic-fat reduction	Imaging (DXA/MRI) indicates preferential loss of visceral and hepatic fat, key for cardiometabolic risk modification. <br/><em>JCM; Radiology</em>
9 Quality of life	Meaningful improvements in satiety, cravings, physical function, and PROs accompany weight/metabolic change. <br/><em>Obesity; Quality of Life Research</em>

2. Molecular Mechanism of Action

2.1 Receptor Pharmacodynamics

GLP-1R: ↓ appetite, ↓ gastric emptying, ↑ glucose-dependent insulin, ↓ glucagon (post-prandial).
GIPR: Amplifies insulin secretion, may enhance adipocyte metabolic flexibility and GI tolerability with GLP-1.
GCGR (glucagon): ↑ energy expenditure and fat oxidation; hepatic lipid mobilization and anti-steatotic effects; modest ↑ hepatic glucose output that is counter-balanced by GLP-1/GIP glycaemic control.

2.2 Down-stream Biology

Pathway	Functional outcome	Context
POMC/AgRP (hypothalamus)	Satiety ↑, cravings ↓	CNS appetite circuits
Islet (GLP-1/GIP)	Glucose-dependent insulin ↑, β-cell stress ↓	Pancreas
Hepatic lipid handling (GCGR)	TG export/oxidation ↑, steatosis ↓	Liver
Brown/white adipose	Thermogenesis/FAO programs ↑	Adipose tissue
CV-renal	BP ↓, natriuresis signals ↑ (weight-mediated + direct)	Vascular/renal

3. Pharmacokinetics

Route: Once-weekly SC injection with dose-escalation to improve GI tolerability.
Absorption/half-life: Engineered for multi-day half-life (~1 week) supporting weekly dosing.
Distribution/clearance: Albumin-binding/acylation prolong exposure; peptide catabolism via proteases; renal/hepatic clearance of fragments.
Food interactions: Not clinically relevant (injected).

4. Pre-clinical and Clinical Evidence

4.1 Obesity (without diabetes)

Dose-ranging Phase 2 showed large, dose-dependent weight loss through 48 weeks, with a majority of participants achieving ≥15% and many ≥20% loss. Trajectories suggested additional loss with continued therapy.

4.2 Type 2 Diabetes

Retatrutide produced robust A1c and weight reductions vs placebo/active comparators, improving fasting/post-prandial glucose, time-in-range (CGM), lipids, and BP. Hypoglycaemia was uncommon outside insulin/sulfonylurea co-use.

4.3 NAFLD/MASH

Meaningful MRI-PDFF reductions and enzyme improvements occurred early, consistent with dual weight-dependent and glucagon-mediated effects; histology programs are ongoing.

Evidence quality note: Data to date are Phase 2 (plus expanding Phase 3 programs). Magnitudes above are representative of published results; long-term outcomes (CV events, MASH histology, hard renal endpoints) are pending.

5. Emerging Clinical Interests

Field	Rationale	Status
Obesity (broad BMI ranges)	Superior weight loss potential	Phase 3
T2D (mono/combination therapy)	Strong A1c + weight effects	Phase 2→3
MASH/NAFLD	Liver-fat and fibrosis pathways	Ongoing trials
OSA	Weight-linked AHI improvement	Exploratory
HFpEF with obesity	Weight/BP/VO₂ & congestion signals	Concept
PCOS/metabolic syndrome	Weight, insulin resistance, ovulatory milieu	Exploratory

6. Safety and Tolerability

Common (dose-related, typically early): Nausea, vomiting, diarrhea/constipation, abdominal pain, transient decreased appetite; generally manageable with gradual titration.
Vitals/labs: Modest HR increase (few bpm); BP decreases; ALT/AST usually fall with weight/liver-fat loss.
Gallbladder: Risk of cholelithiasis/cholecystitis rises with rapid weight loss—monitor symptoms.
Pancreas: Pancreatitis is rare; counsel on symptoms and stop if suspected.
GI motility: Gastroparesis/aspiration risk around anesthesia—follow peri-procedural fasting guidance.
Hypoglycaemia: Uncommon without insulin/secretagogues; adjust those doses as weight and glycaemia improve.
Thyroid C-cell warning (class/rodent): GLP-1–based agents carry a rodent C-cell tumor signal; avoid with personal/family history of MTC or MEN2 pending specific label data.
Contraindications/caution: Pregnancy/breastfeeding, severe GI disease, active gallbladder disease, pancreatitis history—use specialist judgement.

Comparative safety matrix

Feature	Retatrutide (GLP-1/GIP/GCGR)	Tirzepatide (GLP-1/GIP)	Semaglutide (GLP-1)
Weight loss (48–72 wks)	Very high (≥20% avg at upper doses, Phase 2)	High (≈15–22%)	High (≈12–17%)
A1c lowering	~2% (T2D)	~2–2.5%	~1.5–2%
Energy expenditure	↑ (glucagon)	Neutral–mild	Neutral
GI tolerability	GLP-1-like; titration key	GLP-1-like; improved vs GLP-1 alone	GLP-1-class
HR/BP	HR ↑ small; BP ↓	Similar	Similar
NAFLD/MASH	Strong signals	Strong	Strong

7. Regulatory Landscape

Approval status: Investigational; no marketing authorization yet.
Programs: Late-phase obesity and diabetes trials underway; liver-disease programs expanding.
Use outside trials: Not recommended; compounded “tri-agonists” are not equivalent to GMP retatrutide.

8. Future Directions

Cardiovascular-outcomes trial (CVOT) to quantify MACE reduction and renal protection.
Histology-based MASH trials (NASH resolution, fibrosis endpoints).
Body-composition & function: DXA/MRI (visceral/ectopic fat, lean-mass preservation), strength/VO₂.
Dose-finding/titration science to balance maximal efficacy with GI tolerability.
Combination strategies (e.g., statins, SGLT2 inhibitors) and peri-procedural protocols (aspiration risk mitigation).
Patient-reported outcomes on satiety, cravings, and QoL to guide shared decisions.

Selected References

New England Journal of Medicine — Phase 2 retatrutide in obesity: magnitude of weight loss and metabolic effects.
Diabetes Care; JCEM — Glycaemic efficacy and β-cell physiology with incretin/glucagon tri-agonism.
Hepatology; Liver International — Incretin/glucagon pathways in hepatic steatosis and MASH.
Cell Metabolism; Nature Metabolism — Mechanistic work on tri-agonists (energy expenditure, fat oxidation).
Circulation; Atherosclerosis — Cardiometabolic risk-factor changes (BP, lipids, apoB).
Obesity; Quality of Life Research; Chest — PROs, functional outcomes, and OSA signals with substantial weight loss