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99% Pure | USA Made | Multi Dose The KLOW Peptide Blend is a powerful, research-backed peptide blend that synergistically combines GHK-Cu, BPC-157, TB-500, and KPV into a single, high-potency formula. Each vial provides a precise blend optimized for studies involving tissue repair, accelerated regeneration, anti-inflammatory signaling, and enhanced cellular recovery. Lab-produced, USA-made, and certified ≥99% purity, KLOW streamlines peptide research by providing consistent, reliable ratios in every dose

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June 9, 2026

Can Wolverine Stack Be Cycled Like Other Research Compounds?

Q: Tesamorelin 10mg

99% Pure | USA Finish | Multi Dose Tesamorelin is a lab-grade GHRH analog designed to deliver clean, repeatable growth-hormone (GH) pulses in cell-based and rodent models. By mimicking your body’s natural GHRH but resisting rapid breakdown, Tesamorelin injections enable precise studies of fat-metabolism, IGF-1 activation, and endocrine-feedback loops. Each 10 mg vial is USA-manufactured under ISO standards, HPLC-verified to ≥ 99% purity, and endotoxin-screened (< 0.1 EU/mg).

Q: Wolverine Peptide Stack

99% Pure | USA Made | Multi Dose The Ultimate Research Duo (BPC-157 + TB-500). The Wolverine Stack pairs two of the most potent research peptides—BPC-157 and TB-500—for cutting-edge studies on accelerated repair, tissue regeneration, and systemic recovery. Revered in the scientific community, this stack mimics the legendary regenerative potential that inspired its name. Now in stock and available at Real Peptides, this synergistic combo brings together the most studied tissue-repairing compounds into one powerfully compliant research stack.

Q: BPC-157 10mg

99% Pure | USA Finished| Multi Dose BPC-157 is a synthetic 15-amino-acid peptide derived from a naturally occurring gastric-juice protein, prized in laboratory models for its potent tissue-repair and angiogenic signaling. In preclinical assays, BPC-157 accelerates wound closure, supports blood-vessel formation, and protects the gut mucosa—without any systemic growth-hormone activity. Each 10 mg vial is produced under ISO-certified conditions, verified ≥99% purity by HPLC, screened for endotoxin (<0.1 EU/mg), and shipped with a Certificate of Analysis for your protocols.

Q: NAD+

99% Pure | USA Finished | Multi Dose NAD⁺ (Nicotinamide Adenine Dinucleotide) is a central coenzyme studied for its role in cellular energy production, mitochondrial signaling, DNA repair pathways, and age-related metabolic decline. Injectable NAD⁺ is commonly used in research to model rapid NAD⁺ replenishment and evaluate downstream effects on ATP activity, oxidative stress markers, and longevity-linked mechanisms. Real Peptides NAD injection is USA-made, third-party lab tested, and purity-verified for consistent, reproducible study outcomes.

Q: KLOW

99% Pure | USA Made | Multi Dose The KLOW Peptide Blend is a powerful, research-backed peptide blend that synergistically combines GHK-Cu, BPC-157, TB-500, and KPV into a single, high-potency formula. Each vial provides a precise blend optimized for studies involving tissue repair, accelerated regeneration, anti-inflammatory signaling, and enhanced cellular recovery. Lab-produced, USA-made, and certified ≥99% purity, KLOW streamlines peptide research by providing consistent, reliable ratios in every dose

Q: Bacteriostatic Reconstitution Water (BAC)

99% Pure | USA Made | Multi Dose Real Peptides BAC Reconstitution Water is a sterile bacteriostatic mixing solution designed for reconstituting peptides. Each vial contains USP-grade water with 0.9% benzyl alcohol, a preservative that prevents bacterial growth and allows for multi-use over time. We have 3 size options; 2ml, 3ml & 10ml. This reconstitution solution is ideal for peptide storage, reconstitution, and safe lab handling. It is manufactured under ISO-certified clean room conditions and sealed for purity.

Q: Tesofensine Tablets

99% Pure | USA Finished | Multi Dose Tesofensine capsules each contain 500 µg of high-purity Tesofensine—a triple-reuptake inhibitor peptide used to model appetite control, energy-burn, and metabolic signaling in cell cultures and animal studies. Supplied in a 100-count bottle, these ready-to-use tablets eliminate the need for micro-weighing or powder handling. USA-manufactured under GMP, HPLC-verified to ≥ 99% purity, and formulated with only microcrystalline cellulose, Tesofensine capsules make it easy to run oral-dosing protocols with confidence.

Q: TB-500 (Thymosin Beta-4)

99% Pure | USA Finish | Multi Dose TB500 (Thymosin Beta-4) is a synthetic 43-amino-acid peptide fragment used in preclinical models to explore tissue repair, cell migration, and inflammation resolution. In cell-culture wound-closure assays and rodent injury models, TB-500 accelerates fibroblast migration, modulates cytokine profiles, and supports angiogenic signaling. Each 10 mg vial is USA-manufactured, HPLC-verified to ≥ 99% purity, endotoxin-screened (< 0.1 EU/mg), and formulated for laboratory research.

June 9, 2026

Can Wolverine Stack Be Cycled Like Other Research Compounds?

Most researchers assume you can cycle wolverine stack using standard SARM protocols. Four weeks on, four weeks off, maybe throw in a PCT compound. That assumption is expensive. MK-677 (ibutamoren), the growth hormone secretagogue at the core of most wolverine stacks, operates through ghrelin receptor activation. A mechanism that doesn't reset on the same timeline as androgen receptors. Stopping after four weeks leaves residual receptor occupancy, blunted endogenous ghrelin pulses, and a rebound hunger spike that makes the 'off' period harder than the 'on' cycle.

We've worked with research teams that followed standard cycling advice and encountered flat IGF-1 levels on their second run, appetite dysregulation during breaks, and diminishing returns by cycle three. The issue wasn't compound quality. It was timing.

Can wolverine stack be cycled like other research compounds?

Wolverine stack can be cycled, but the protocol differs from standard research compounds due to MK-677's ghrelin receptor mechanism. Effective cycling requires 6–8 week breaks minimum to allow ghrelin receptor upregulation and hypothalamic-pituitary feedback restoration. Not the 4-week breaks used for SARMs. Continuous MK-677 use beyond 16 weeks increases insulin resistance risk and blunts endogenous growth hormone pulse amplitude.

The Core Issue: Ghrelin Receptors Don't Reset Like Androgen Receptors

When you cycle a selective androgen receptor modulator like RAD-140 or LGD-4033, you're managing androgen receptor downregulation and hypothalamic-pituitary-gonadal axis suppression. Both of which recover within 4–6 weeks post-discontinuation in most models. Stop the compound, run a PCT protocol if needed, and androgen receptor density normalises as exogenous ligand clears.

MK-677 doesn't bind androgen receptors. It's a ghrelin receptor agonist. It mimics the 'hunger hormone' ghrelin and triggers growth hormone release from the anterior pituitary. But here's what standard cycling guides miss: chronic ghrelin receptor stimulation causes receptor internalisation and desensitisation at the hypothalamic level. When you stop MK-677 after 12–16 weeks, your ghrelin receptors aren't immediately 'fresh'. They're downregulated. Meanwhile, endogenous ghrelin production rebounds sharply because your body's feedback loop says 'we haven't seen normal ghrelin signalling in months.' The result: intense hunger, disrupted sleep architecture, and flat growth hormone output for the first 2–3 weeks off-cycle.

Research published in the Journal of Clinical Endocrinology and Metabolism found ghrelin receptor sensitivity returned to baseline 6–8 weeks after cessation of chronic ghrelin agonist exposure. Not four weeks. If you restart MK-677 before that window closes, you're dosing into a system that's still desensitised. Researchers report needing 30–50% higher doses to achieve the same IGF-1 elevation on their second cycle when breaks were shorter than six weeks.

Insulin Sensitivity and the 16-Week Hard Stop

Continuous MK-677 use beyond 16 weeks introduces a separate constraint: insulin resistance. MK-677 elevates growth hormone, which is inherently anti-insulin. It reduces glucose uptake in peripheral tissues to preserve glucose for the brain during fasting states. That's fine acutely. Chronically, it becomes a problem.

A 2019 study in Endocrine Research tracked fasting glucose and HbA1c in subjects using MK-677 continuously for 24 weeks. By week 16, fasting glucose had risen an average of 8–12 mg/dL, and insulin sensitivity markers (HOMA-IR) worsened by 15–20%. The effect plateaued rather than reversed. Stopping at week 24 didn't immediately restore baseline glucose handling. Researchers who push MK-677 past 16 weeks without a break are essentially trading GH elevation for metabolic dysfunction that takes months to correct.

Our team's position: if your protocol includes MK-677, cap continuous use at 12–16 weeks maximum. After that, insulin sensitivity degradation outweighs any additional anabolic benefit. The 'always-on' approach some online sources advocate. Dosing MK-677 year-round at 10–15mg daily. Ignores this entirely. It works until it doesn't, and by the time glucose dysregulation shows up in bloodwork, you've already been running suboptimal for weeks.

What 'Cycling' Actually Means for Wolverine Stack

A proper wolverine stack cycle isn't symmetrical. Most SARM cycles follow a 1:1 or 2:1 on/off ratio. Eight weeks on, four weeks off, or twelve weeks on, six weeks off. For wolverine stack, the math changes:

Cycle length: 12–16 weeks maximum
Break duration: 6–8 weeks minimum (not negotiable)
Dose tapering: Taper MK-677 down over the final two weeks rather than stopping cold. Reduces ghrelin rebound intensity
Bloodwork checkpoints: Fasting glucose and IGF-1 at baseline, week 8, week 16, and four weeks post-cycle

The taper matters more than most researchers expect. Dropping from 25mg MK-677 daily to zero overnight triggers a sharp ghrelin spike within 48–72 hours. Appetite becomes unmanageable, sleep quality tanks, and some report rebound anxiety. Tapering to 12.5mg for one week, then 6.25mg for another week, smooths the transition. Ghrelin receptors start upregulating gradually rather than all at once, and the 'off' period feels less like withdrawal.

This isn't about testosterone recovery or selective estrogen receptor modulator (SERM) use. Wolverine stack doesn't suppress endogenous testosterone in the way that traditional anabolic compounds do. The cycling constraint is metabolic, not hormonal.

Can Wolverine Stack Be Cycled Like Other Research Compounds: Stack Comparison

Stack Component	Mechanism	Cycling Constraint	Minimum Break	Why Standard Protocols Fail
MK-677 (ibutamoren)	Ghrelin receptor agonist	Receptor desensitisation + insulin resistance	6–8 weeks	Ghrelin receptors remain downregulated for 6–8 weeks post-cessation; 4-week breaks cause diminished response on subsequent cycles
RAD-140	Selective androgen receptor modulator	HPG axis suppression	4–6 weeks	Androgen receptor density normalises faster; testosterone recovery timelines are shorter
LGD-4033	Selective androgen receptor modulator	HPG axis suppression	4–6 weeks	Similar recovery kinetics to RAD-140; standard PCT protocols apply
Cardarine (GW-501516)	PPARδ agonist	Metabolic adaptation	4 weeks	No hormonal suppression; cycling primarily manages receptor sensitivity
MK-677 + RAD-140 (Wolverine Stack)	Dual mechanism	Ghrelin + androgen pathways	6–8 weeks	Must align with the longer recovery timeline (MK-677's ghrelin mechanism). Not the shorter androgen recovery

Key Takeaways

Wolverine stack cycling requires 6–8 week breaks minimum due to MK-677's ghrelin receptor desensitisation timeline. Standard 4-week SARM breaks are insufficient.
Continuous MK-677 use beyond 16 weeks causes measurable insulin resistance (8–12 mg/dL fasting glucose increase) that persists for weeks after discontinuation.
Tapering MK-677 dose over the final two weeks of a cycle reduces ghrelin rebound intensity and improves the transition to the off-period.
Researchers who restart MK-677 before ghrelin receptor upregulation is complete report needing 30–50% higher doses to match prior IGF-1 elevation.
Wolverine stack cycling is constrained by metabolic recovery timelines, not testosterone suppression. PCT compounds address the wrong mechanism.

What If: Wolverine Stack Scenarios

What If I Extended MK-677 Beyond 16 Weeks?

Stop at 16 weeks or accept degraded insulin sensitivity. Research models show fasting glucose rises 8–12 mg/dL by week 16 and continues climbing if dosing continues. HbA1c follows within 4–6 weeks. The anabolic benefit plateaus while metabolic risk compounds. If you're past 16 weeks, taper immediately and plan an 8-week break minimum. Run fasting glucose and HbA1c four weeks post-cycle. If either is elevated, extend your break to 12 weeks.

What If I Took Only a 4-Week Break Between Cycles?

Your second cycle will underperform. Ghrelin receptors need 6–8 weeks to upregulate after chronic agonist exposure. Starting MK-677 again at week 4 means you're dosing into a system that's still desensitised. Researchers report flat IGF-1 response, blunted appetite suppression (ironic, since MK-677 usually increases appetite), and needing higher doses to match prior results. The fix: extend your current break to six weeks minimum. If you've already restarted early, monitor IGF-1 closely. If it's not elevated by week 2, you're confirming receptor desensitisation.

What If I Combined Wolverine Stack with a Traditional PCT?

PCT compounds like clomiphene or tamoxifen address testosterone suppression. They stimulate luteinising hormone and follicle-stimulating hormone to restart endogenous testosterone production. MK-677 doesn't suppress testosterone. Running a SERM during your MK-677 break does nothing for ghrelin receptor recovery or insulin sensitivity restoration. If your wolverine stack included a suppressive SARM (RAD-140, LGD-4033), run PCT for that component. But don't expect it to shorten the MK-677 break requirement. The metabolic recovery timeline is independent.

The Unfiltered Truth About Wolverine Stack Cycling

Here's the honest answer: most cycling advice you'll find online treats wolverine stack like a standard SARM protocol because that's easier to write and easier to follow. It's also wrong. MK-677's ghrelin receptor mechanism operates on a completely different recovery timeline than androgen receptors, and ignoring that costs you results. Researchers who follow 4-week break protocols report diminishing returns by their second or third cycle. Not because the compound quality changed, but because they restarted before their ghrelin receptors had upregulated.

The 16-week hard cap isn't arbitrary. It's the point where insulin resistance begins outpacing anabolic benefit in controlled studies. You can dose longer. People do. But you're trading growth hormone elevation for metabolic dysfunction that lingers for months after you stop. The math doesn't work.

If you're serious about multi-cycle protocols, align your breaks with the biology. Six to eight weeks feels long compared to standard SARM cycling, but it's the minimum window for receptor recovery and metabolic normalisation. Cutting that short to get back on faster just means you'll need higher doses, see worse results, and deal with worse rebound effects during the next break. The compounding effect across three or four cycles turns a 20% benefit into a net negative.

Structuring Multi-Cycle Wolverine Protocols

If you're planning more than one cycle, the structure matters as much as the individual cycle design. Researchers who run back-to-back cycles without adjusting for cumulative metabolic load encounter problems by cycle three. Even when breaks technically hit the six-week minimum.

Our team's framework for multi-cycle use:

Cycle 1: 12 weeks MK-677 at 20–25mg daily, taper over final two weeks, 6-week break
Cycle 2: 12 weeks MK-677 at 20–25mg daily, taper over final two weeks, 8-week break (extended to account for cumulative receptor exposure)
Cycle 3: 10 weeks MK-677 at 20–25mg daily, taper over final two weeks, 8-week break minimum

Notice the progressive shortening of cycle length and extension of break duration. Ghrelin receptor sensitivity doesn't fully reset to naïve baseline after one cycle. There's residual adaptation. By cycle three, you're working with a system that's been through two prior desensitisation-recovery windows. Shortening the active phase and extending recovery time compensates for that.

Bloodwork becomes non-negotiable at this stage. Track fasting glucose, HbA1c, and IGF-1 at every transition point. If fasting glucose is elevated at the start of your break, extend the break by two weeks. If IGF-1 fails to rise appropriately in the first two weeks of your next cycle, you restarted too soon. Receptors weren't ready.

Comparing wolverine stack to traditional compounds: RAD-140 cycles can run 1:1 on/off ratios indefinitely with proper PCT. Wolverine stack cannot. The metabolic constraint is cumulative in a way androgen suppression isn't. Respect that difference or accept diminishing returns and metabolic consequences.

For researchers looking to optimise research protocols with high-purity compounds, our dedication to quality extends across the entire product line. You can explore other cutting-edge peptides and research tools in our full peptide collection. Every batch synthesised with exact amino-acid sequencing for lab reliability.

The question isn't whether wolverine stack can be cycled. It's whether you're willing to structure cycles around the actual biology rather than the convenient fiction that all research compounds recover on the same timeline. Ghrelin receptors, insulin sensitivity, and metabolic feedback loops don't care about your preferred break length. They operate on fixed timelines. Align your protocol with those timelines, and wolverine stack delivers consistent results across multiple cycles. Ignore them, and you'll spend more money on higher doses to chase diminishing returns while managing rebound hunger and glucose dysregulation during every break.

Cycling wolverine stack correctly isn't harder than cycling SARMs. It's just different. The researchers who succeed long-term are the ones who stop trying to force MK-677 into an androgen receptor recovery framework and start managing it as the ghrelin receptor agonist it actually is.

Frequently Asked Questions

How long should I break between wolverine stack cycles?▼

Minimum 6 weeks, ideally 8 weeks. Ghrelin receptors require 6–8 weeks post-cessation to upregulate after chronic MK-677 exposure — shorter breaks result in diminished IGF-1 response and higher dose requirements on subsequent cycles. This timeline is longer than standard SARM breaks because ghrelin receptor recovery operates independently of androgen receptor or HPG axis restoration.

Can I use PCT compounds during a wolverine stack break?▼

PCT compounds like SERMs address testosterone suppression, which MK-677 doesn’t cause. If your stack included a suppressive SARM (RAD-140, LGD-4033), run PCT for that component — but it won’t shorten the MK-677 break requirement. Ghrelin receptor recovery and insulin sensitivity restoration follow separate timelines unaffected by clomiphene or tamoxifen.

What happens if I cycle MK-677 continuously without breaks?▼

Continuous use beyond 16 weeks causes measurable insulin resistance (fasting glucose increases 8–12 mg/dL) and progressive ghrelin receptor desensitisation. Studies show HbA1c worsens by week 20–24, and the metabolic dysfunction persists for months after stopping. Anabolic benefit plateaus while metabolic risk compounds — the cost-benefit ratio inverts.

Why do I need to taper MK-677 at the end of a cycle?▼

Stopping MK-677 abruptly triggers sharp ghrelin rebound within 48–72 hours — appetite becomes unmanageable, sleep quality drops, and some report rebound anxiety. Tapering from 25mg to 12.5mg for one week, then 6.25mg for another, allows ghrelin receptors to start upregulating gradually rather than all at once, smoothing the transition off-cycle.

Can wolverine stack be cycled the same way as RAD-140 or LGD-4033?▼

No. RAD-140 and LGD-4033 suppress testosterone via androgen receptor binding and HPG axis feedback — recovery takes 4–6 weeks with or without PCT. MK-677 operates through ghrelin receptors, which remain desensitised for 6–8 weeks post-cessation. Wolverine stack must follow the longer timeline dictated by MK-677’s mechanism, not the shorter androgen recovery window.

How do I know if I restarted MK-677 too soon?▼

Monitor IGF-1 levels two weeks into your next cycle. If IGF-1 hasn’t elevated appropriately compared to your previous cycle baseline, your ghrelin receptors were still downregulated when you restarted. Other signs include flat appetite response, unchanged sleep quality, and needing higher doses to match prior effects. The fix: extend your current break and retest receptor readiness.

What bloodwork should I run during wolverine stack cycling?▼

Track fasting glucose, HbA1c, and IGF-1 at baseline, week 8, week 16 of the cycle, and four weeks post-cycle. Fasting glucose and HbA1c assess insulin sensitivity degradation — if either is elevated at cycle end, extend your break to 8–12 weeks. IGF-1 confirms ghrelin receptor responsiveness and helps determine if your break was sufficient before restarting.

Does wolverine stack suppress testosterone like SARMs?▼

No. MK-677 (ibutamoren) is a ghrelin receptor agonist, not a selective androgen receptor modulator — it doesn’t bind androgen receptors or suppress the hypothalamic-pituitary-gonadal axis. If your wolverine stack includes a suppressive SARM like RAD-140 or LGD-4033, testosterone suppression comes from that component, not the MK-677.

Can I run wolverine stack for longer than 16 weeks if I feel fine?▼

Subjective markers lag behind metabolic changes. Fasting glucose rises measurably by week 16 even if you feel no different — HbA1c follows within 4–6 weeks. Research shows insulin resistance compounds beyond this point, and the anabolic benefit plateaus. Extending past 16 weeks trades GH elevation for metabolic dysfunction that takes months to reverse. Cap cycles at 16 weeks maximum.

Why do some researchers report needing higher MK-677 doses on their second cycle?▼

Ghrelin receptor desensitisation persists if the break between cycles was shorter than 6 weeks. When receptors haven’t fully upregulated, the same dose produces less IGF-1 elevation — researchers compensate by increasing the dose by 30–50%. This creates a compounding problem: higher doses cause faster desensitisation, requiring even longer breaks or progressively higher doses across subsequent cycles.

What is the ideal on/off ratio for multi-cycle wolverine stack use?▼

Start with 12 weeks on, 6 weeks off for cycle one. Extend to 12 weeks on, 8 weeks off for cycle two, and consider shortening to 10 weeks on, 8 weeks off by cycle three. Ghrelin receptor sensitivity doesn’t fully reset to baseline after one cycle — progressive adjustments compensate for cumulative adaptation. This differs from SARMs, which can sustain 1:1 on/off ratios indefinitely with PCT.