Cagrilintida

Cagrilintida

Rango de precios: entre 590,00 $ y 975,00 $

 Envío gratuito para pedidos superiores a 2.000 $

Precios por volumen

Precio por envase (10 viales). El descuento se aplica únicamente a este compuesto; no se admiten combinaciones.

5 mg
Cantidad Precio por paquete Ahorros
1 paquete $590 per pack
2 paquetes $502 per pack 15 % de descuento
3 paquetes $426 per pack 28 % de descuento
5 paquetes $384 per pack 35 % de descuento
10 paquetes $345 per pack 42 % de descuento
25 paquetes $311 per pack 47 % de descuento
10 mg
Cantidad Precio por paquete Ahorros
1 paquete $975 per pack
2 paquetes $829 per pack 15 % de descuento
3 paquetes $704 per pack 28 % de descuento
5 paquetes $634 per pack 35 % de descuento
10 paquetes $571 per pack 41 % de descuento
25 paquetes $514 per pack 47 % de descuento

Cagrilintide — Long-Acting Amylin / Calcitonin Receptor Dual Agonist (DACRA)

Cagrilintide (AM833) is a long-acting synthetic analog of amylin — the pancreatic beta-cell hormone co-secreted with insulin in response to nutrient intake. Structurally derived from pramlintide (the first approved amylin analog) with strategic amino acid substitutions at positions N14E, V17R, and P37Y, plus lipidation of the N-terminal lysine, cagrilintide achieves resistance to amyloid fibril formation, extended plasma half-life, and once-weekly dosing compatibility. Critically, these modifications make it a non-selective dual agonist at both amylin receptors (AMY1R, AMY3R) and the calcitonin receptor (CTR) — classifying it as a Dual Amylin and Calcitonin Receptor Agonist (DACRA) with a broader pharmacological profile than its predecessor.

Cagrilintide occupies a unique position in the metabolic research landscape: it acts on an entirely different receptor system than GLP-1R, GIPR, and GcgR agonists, engaging brainstem satiety pathways that are anatomically and mechanistically distinct from hypothalamic incretin signaling. This makes it both a standalone research compound of significant interest and a synergistic partner to GLP-1R agonists — a combination under active Phase 3 investigation as CagriSema (cagrilintide + semaglutide).

Why Amylin / Calcitonin Dual Receptor Agonism Matters

The amylin receptor system has long been recognized as a physiologically critical but pharmacologically underexploited satiety pathway. Native amylin acts primarily through the caudal hindbrain — specifically the area postrema (AP) and nucleus tractus solitarius (NTS) — rather than the hypothalamic arcuate nucleus that GLP-1 primarily targets. This neuroanatomical separation means amylin and GLP-1 receptor agonism engage satiety through both distinct and overlapping central circuits, with documented additive effects when both pathways are activated simultaneously.

Receptor / Pathway Efectos de la investigación primaria
AMY1R (Amylin Receptor 1) Brainstem-mediated satiety signaling, meal-ending satiation, food intake reduction via area postrema and NTS
AMY3R (Amylin Receptor 3) Body weight regulation, energy balance modulation — confirmed as primary mediator of cagrilintide’s weight-lowering effects in knockout studies
CTR (Calcitonin Receptor) Complementary metabolic signaling; co-activation with AMYRs via DACRA profile may contribute to adipose and glucose effects distinct from selective amylin agonism
Gastric Emptying Slowing of gastric emptying via brainstem pathways — mechanistically overlapping with but neurally distinct from GLP-1R-mediated gastric motility effects
Glucagon Suppression Postprandial glucagon inhibition, contributing to glucose homeostasis independently of insulin secretion pathway
Hedonic / Reward Pathways Engagement of both homeostatic and hedonic brain regions — a dual-circuit satiety profile that distinguishes amylin signaling from purely hypothalamic appetite suppression

Aplicaciones de investigación

Cagrilintide is used in studies examining:

  • Brainstem amylin receptor biology and the specific contributions of AMY1R vs. AMY3R to body weight regulation and food intake control
  • DACRA pharmacology — the mechanistic differences between selective amylin agonism and non-selective amylin/calcitonin receptor co-activation
  • Additive and synergistic satiety effects when combined with GLP-1R agonists, particularly in dual-pathway appetite suppression models
  • Gastric emptying dynamics and their independent contribution to glucose regulation vs. GLP-1R-mediated effects
  • Postprandial glucagon suppression via amylin receptor vs. GLP-1R pathways — distinguishing their relative contributions
  • Body composition endpoints under sustained once-weekly amylin receptor stimulation
  • Central nervous system satiety circuitry — homeostatic (hypothalamic) vs. hedonic (reward) pathway engagement
  • Comparative efficacy benchmarking against GLP-1R mono-agonists, dual incretin agonists, and combination CagriSema protocols

Especificaciones
Formato Polvo liofilizado
Pureza ≥99%
Alias AM833, CagriSema component (when combined with semaglutide)
Tallas disponibles 5mg · 10mg
Almacenamiento 2–8 °C sin abrir; estable durante más de 12 meses
Uso Solo para fines de investigación — No apto para uso humano

Reconstitución

Cagrilintide arrives as lyophilized powder and must be reconstituted with bacteriostatic water prior to use. Use the formula:

Total en mg ÷ Volumen añadido (mL) = Concentración (mg/mL)

Ejemplo: vial de 5 mg + 2 ml de agua destilada = solución de 2,5 mg/ml

El péptido reconstituido debe conservarse a una temperatura de entre 2 y 8 °C y utilizarse en un plazo de 28 a 30 días.

Notas sobre el protocolo

Cagrilintide’s long half-life and once-weekly dosing profile make it one of the more practical amylin analogs for sustained research protocols. Dose escalation is standard in research designs to characterize the dose-response curve and observe receptor adaptation, particularly for GI-related endpoints that tend to attenuate with continued exposure.

Esquema típico de titulación:

  • Starting dose: 0.25–0.5mg per administration
  • Aumento gradual: Aumentar la dosis entre 0,25 y 0,5 mg cada 2-4 semanas, según la tolerancia del paciente.
  • Frequency: Once weekly
  • Combination protocols: Frequently co-administered with semaglutide or other GLP-1R agonists to study additive/synergistic appetite suppression across dual neural satiety circuits
  • Study duration: 12–20 weeks for body composition and metabolic endpoints

Efectos observados con frecuencia en modelos de investigación:

  • GI-related (receptor-mediated, typically transient): Nausea, vomiting, decreased appetite, early satiety, constipation — most pronounced during dose escalation; generally attenuate with continued dosing as receptor adaptation occurs
  • Metabolic: Dose-dependent reductions in food intake and body weight; postprandial glucagon suppression; fluid balance shifts at higher doses
  • Other: Injection site reactions; headache; mild dizziness — profile broadly comparable to GLP-1R agonists given overlapping GI receptor engagement

Pilas de investigación

Cagrilintide is commonly paired in research settings with:

  • Semaglutide — Cagrilintide is a long-acting amylin analogue acting on area postrema and hypothalamic amylin receptors; Semaglutide acts on GLP-1 receptors. Dual-receptor engagement across amylin and incretin axes is the basis of the CagriSema combination studied in clinical metabolic research.
  • Tirzepatide — Tirzepatide’s dual GLP-1/GIP agonism is studied alongside Cagrilintide to assess triple-pathway coverage (amylin + GLP-1 + GIP) in energy homeostasis models.
  • CJC-1295 No DAC / Ipamorelin — This GHRH/ghrelin receptor blend is paired with Cagrilintide in research models examining concurrent modulation of metabolic and growth hormone secretion axes.

Garantía de pureza

Cada lote tiene una pureza ≥99 %. Si sometes tu compuesto a un análisis independiente y los resultados no coinciden, envíanos el certificado de análisis (COA) y te concederemos un vale de compra sin hacerte preguntas.

  • Kits de investigación de 10 viales: cada pedido incluye un kit completo de 10 viales liofilizados para protocolos de investigación prolongados
  • Formato liofilizado: todos los péptidos se suministran liofilizados en viales estériles sellados para garantizar la máxima estabilidad y vida útil.
  • Calidad farmacéutica: pureza superior al 99 %, verificada mediante ensayos independientes; certificados de análisis disponibles previa solicitud
  • Almacenamiento refrigerado: conserve los viales sin abrir a una temperatura de entre 2 y 8 °C (36-46 °F) para garantizar una estabilidad óptima; la vida útil es de más de 12 meses si se almacena correctamente.
  • Se requiere reconstitución: debe mezclarse con agua bacteriostática antes de su uso.
  • Estéril y sellado: cada vial está sellado individualmente para mantener la esterilidad hasta que esté listo para su reconstitución
  • Solo para uso en investigación: se vende exclusivamente con fines de investigación científica y de laboratorio; no apto para el consumo humano

 

Productos relacionados

0