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Richard A. Loy US
I wish I had found this when I started. Things I learned the hard way and that you shouldn't do with Retatrutide: 1- Not drinking enough fluids and not including mineral salts and electrolytes. You dehydrate very quickly with Retatrutide. 2- Cutting calories by more than 1000 kcal was crazy, and I lost almost as much muscle as fat. Remember that Retatrutide increases your basal metabolic rate. 3- Not getting enough protein (I always did this correctly, but many people make mistakes). Aim for 2 grams per kilogram of body weight of muscle mass. 4- Starting with very high doses or increasing them too quickly. I was cautious and started with 0.5 mg and then spent 4 weeks on 1 mg. 5- Thinking it's Tirze or Sema; it's not the same at all. Appetite suppression is less pronounced, and Retatrutide works in the long term. 6- Not weight training; this is a very common mistake. I love it, but a lot of people make mistakes here. I think that training, along with protein, is vital for maintaining mu
04.22.2026 5
Retatrutid 1kits(10Vials)
Larry K. Goheen US
32M - Athletic/sports background - I have done about 2-3 days per week lifting/cardio: 30min-1hr. Not strict with it. I went from 2-4-6-8 each month and I've stayed at 8mg. Mots at 2mg 3x weekly. My diet consists of mostly protein and complex carbs. both healthy and unhealthy sources. I don't count calories. Tbh for being as inconsistent as I've been with diet and training, I'm surprised and content with these results. Reta is a most excellent tool!
04.09.2026 7
Retatrutid 1kits(10Vials)
Albert US
I have been on Retatrutide since January. I have been on Semaglutide and Trizepitide in the past under brand names. I have found Reta, and it’s worked the best for me. I have lost 37 pounds using Reta without the monthly increases that are within the studies. It doesn’t make me feel miserable. I have experience very very minimal side effects. And honesty I can’t see myself ever changing.
04.09.2026 7
Retatrutid 1kits(10Vials)
Martin Lucas US
Hey all. I started retatrutide through a friend about 4 months ago and the success has been astounding. I've lost 60 lbs so far (267-208 as of today) and feel much better about myself and the progress I've made in multiple facets of life. I found this place and have been lurkin for a while just taking information in and figured I'd finally post something. Thank you all for the valuable insight and for more to come.
04.06.2026 6
Retatrutid 1kits(10Vials)
Vivian C. Walsh US
I have been taking retatrutide for a few weeks and I had the effects (atleast the weight loss mainly) (hard to say if it was mainly from the hard work put in though) I have already purchased the goods from SH., I was using 13mm needles and now I have some 12.7mm ones (the ones supplied from UK pharmacies) I was wondering if these are too large/long - I know a lot of people use 8mm, could I just choose not to insert the whole needle? Or what angle would be best, I do have a decent amount of belly fat so I believe angled the 12.7mm should work - just wondering if any advice ! Thanks
02.25.2026 5
Retatrutid 1kits(10Vials)
Carlos US
This was my 6th order with SH, arrived in 8 days to the UK, as standard for them. I am delighted.
02.12.2026 4
Retatrutid 1kits(10Vials)
Source: PubChem
Figure 1 Model of parathyroid hormone (PTH)/teriparatide and PTH-related peptide (PTHrP/abaloparatide activation of parathyroid hormone type 1 receptor (PTH1R))
[4]. Effects on Cartilage Metabolism (in Osteoarthritis-Related Studies) Promotes Cartilage Matrix Synthesis: Studies in osteoarthritis (OA) have demonstrated that abaloparatide exerts a protective effect on cartilage. Articular chondrocytes express PTH1R, and Abaloparatide activates this receptor, stimulating chondrocytes to synthesize components of the cartilage matrix. For example, studies indicate Abaloparatide increases lubricin (Prg4) expression, an important extracellular matrix protein in cartilage that is crucial for maintaining joint lubrication and reducing friction. It also promotes synthesis of type II collagen, the primary component of cartilage matrix, which helps maintain cartilage structural and functional integrity. By increasing synthesis of these cartilage matrix components, Abaloparatide aids in repairing and protecting damaged cartilage tissue, slowing the progression of osteoarthritis
[5]. Inhibiting chondrocyte hypertrophy and degeneration: Abaloparatide can suppress the hypertrophic differentiation process of chondrocytes. During osteoarthritis progression, chondrocytes undergo hypertrophic differentiation, characterized by increased cell volume and elevated expression of specific hypertrophy markers such as type X collagen (Col10). This process leads to degradation of the cartilage matrix and cartilage degeneration. Studies indicate that Abaloparatide treatment alleviates the upregulation of Col10 expression in cartilage tissue while reducing the number of large hypertrophic-like cells. This suggests it can slow chondrocyte hypertrophic differentiation, maintain the normal chondrocyte phenotype, thereby protecting cartilage and delaying osteoarthritis progression
[5].
What are the applications of Abaloparatide? Osteoporosis Treatment Postmenopausal Osteoporosis: Abaloparatide, a selective agonist of the parathyroid hormone receptor 1 (PTHR1), is indicated for treating osteoporosis, particularly in postmenopausal women at fracture risk or unresponsive to other therapies. It significantly increases bone mineral density and reduces the incidence and risk of new vertebral and non-vertebral fractures in postmenopausal women. Male Osteoporosis: In Chandler H's study on male osteoporosis using orchidectomized rats (ORX rats, a male osteoporosis model), Abaloparatide treatment resulted in greater increases in BMD measured by dual-energy X-ray absorptiometry (DXA) and peripheral quantitative computed tomography (pQCT) at sites including the total body, lumbar spine, femur, and tibia. It significantly improved trabecular formation, bone volume, and microarchitecture without increasing osteoclast numbers. This suggests Abaloparatide holds potential therapeutic benefits for male osteoporosis
[6]. Post-Traumatic Osteoarthritis (PTOA) Treatment: Following knee PTOA induction via medial meniscus destabilization (DMM) surgery in 16-week-old male C57BL/6 mice, daily subcutaneous injections of 40 μg/kg Abaloparatide (or saline as control) were administered starting 2 weeks post-surgery for 6 weeks. Tissue analysis was performed at 8 weeks. Results showed that compared to the saline-treated group, the Abaloparatide-treated group exhibited reduced DMM-induced articular cartilage loss and preserved tibial surface cartilage tissue. Immunohistochemical analysis revealed that Abaloparatide treatment mitigated the upregulation of type X collagen (Col10) in cartilage, increased lubricin (Prg4) expression in non-calcified cartilage areas, and reduced the number of large hypertrophic cells. suggesting that Abaloparatide slows hypertrophic differentiation and exerts a chondroprotective effect in mouse PTOA, offering a novel therapeutic strategy for PTOA
[5]. Alveolar Bone Regeneration: Post-extraction alveolar bone resorption severely impedes subsequent orthodontic tooth movement (OTM) or implant placement. Tan B synthesized biodegradable, bifunctional bioactive calcium phosphate nanoblossoms (NFs) loaded with Abaloparatide (ABL), termed ABL@NFs. This material exhibits a porous layered structure, high drug encapsulation efficiency, and excellent biocompatibility. ABL was initially released to recruit stem cells, followed by sustained release of Ca⊃2;⁺ and PO₄⊃3;⁻ for in situ interfacial mineralization. This successfully restored morphologically and functionally active alveolar bone without compromising OTM
[7]. Refractory Hypoparathyroidism (HPT): Chamseddin R reported a 39-year-old female with iatrogenic HPT who failed to achieve normal serum calcium levels despite high-dose vitamin D, calcium supplements, and recombinant PTH (rPTH) injections. Following subcutaneous administration of abaloparatide via the Simplicity patch with close monitoring and personalized dosing, her serum calcium remained stable at 9 mg/dL after 2 months. By 4 months, she maintained normal serum calcium without hypocalcemia episodes while gradually reducing oral calcium and vitamin D supplementation
[3]. Promoting Spinal Fusion: In cervical-thoracic revision surgery, abaloparatide was used to promote spinal fusion in patients with a history of cervical instability and multiple failed cervical surgeries. Parikh S et al. reported a 66-year-old female patient who initiated daily 80 mcg Abaloparatide treatment two weeks postoperatively for a planned 12-week course. Cervical CT scans at 3 and 6 months demonstrated well-healed cervical-thoracic fusion with no signs of nonunion
[8].
Conclusion Abaloparatide's clinical application centers on osteoporosis treatment. It is indicated for postmenopausal women with osteoporosis at high fracture risk or unresponsive to other therapies, significantly increasing bone mineral density (BMD) and reducing vertebral and non-vertebral fracture risk. For male osteoporosis, animal studies demonstrate increased BMD at multiple sites and improved bone microarchitecture, indicating potential therapeutic value. In post-traumatic osteoarthritis, it reduces cartilage loss and inhibits chondrocyte hypertrophy to protect cartilage. In alveolar bone regeneration, ABL@NFs materials loaded with this drug promote bone regeneration, offering a solution for post-orthodontic bone repair. Research also supports its use in refractory hypoparathyroidism and spinal fusion promotion.
About The Author The above-mentioned materials are all researched, edited and compiled by Cocer Peptides.
Scientific Journal Author Bin T is a researcher at the Department of Chemistry, Peking University, specializing in nanomaterials and their applications in biomedical engineering. His work focuses on the design and synthesis of functional nanostructures for targeted drug delivery and tissue regeneration. Tan has co-authored numerous publications in leading scientific journals, contributing to advancements in nanomedicine and regenerative therapies. Bin T is listed in the reference of citation [7].
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