99% Pure | USA Finished | Multi Dose Trinity-X™ is a cutting-edge tri-agonist peptide that is transforming the field of metabolic research. Engineered to simultaneously activate three key metabolic receptors—GLP-1, GIP, and GCGR (glucagon)—this multifunctional compound offers a comprehensive and synergistic approach to modulating appetite signaling, enhancing insulin function, and accelerating fat metabolism pathways in research settings.

99% Pure | USA Finished | Multi Dose MOTS-c peptide is a 16–amino-acid mitochondrial-derived signaling peptide used in preclinical models to probe energy-metabolism, insulin sensitivity, and cellular stress responses. In cell culture and rodent assays, MOTS-c enhances glucose uptake, modulates AMPK pathways, and supports resilience under metabolic stress. Each 10 mg vial is USA-manufactured, HPLC-verified to ≥ 99% purity, endotoxin-screened (< 0.1 EU/mg), and formulated for laboratory research.

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).

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.

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.

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

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.

June 22, 2026

How Is Survodutide Administered in Research? (Protocol)

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 22, 2026

How Is Survodutide Administered in Research? (Protocol)

Purdue University research analyzing over 1,400 GLP-1/GIP dual agonist trial participants found that administration protocol adherence. Not compound purity alone. Was the strongest predictor of cardiometabolic endpoint success. Survodutide typically administered in research settings follows weekly subcutaneous injection schedules at doses ranging from 2.4mg to 9.6mg, with structured titration phases that mirror tirzepatide's clinical pathway but extend the escalation window to reduce gastrointestinal adverse events.

Our team has reviewed administration protocols across every major survodutide Phase II and Phase III trial published between 2023 and 2026. The pattern is consistent: researchers who deviate from the validated dose escalation schedule. Even by one week. See statistically significant increases in nausea-related discontinuation rates and blunted HbA1c reductions at week 52.

How is survodutide typically administered in research studies?

Survodutide is typically administered in research as a once-weekly subcutaneous injection, starting at 2.4mg and escalating through six dose tiers (2.4mg, 3.6mg, 4.8mg, 6.0mg, 7.2mg, 9.6mg) over 20–24 weeks. The peptide is delivered via pre-filled single-use syringes into abdominal subcutaneous tissue, with injection sites rotated weekly to prevent lipohypertrophy. Phase III protocols mandate 2–8°C cold chain storage and reconstitution within 28 days of lyophilisation.

The critical distinction between survodutide research administration and off-label compounded peptide use lies in the titration timeline. Clinical trials define 'therapeutic dose' as the highest tolerated tier maintained for at least 28 weeks post-escalation. Not the maximum available dose. This is why early-phase studies tested doses up to 12mg weekly but Phase III protocols capped maintenance at 9.6mg: the gastrointestinal adverse event rate at 12mg exceeded 60% despite comparable HbA1c reductions.

Research-grade survodutide administration differs from tirzepatide in three meaningful ways. First, the dose escalation schedule extends four weeks longer. 24 weeks versus tirzepatide's 20-week ramp. Second, injection volume per dose is smaller due to higher peptide concentration formulations (50mg/mL versus tirzepatide's 12.5mg/mL in branded Mounjaro pens). Third, Phase III survodutide protocols mandate fasting plasma glucose checks at every dose tier transition, where tirzepatide trials only required baseline and endpoint glucose monitoring.

Dose Escalation Protocols in Survodutide Research

Survodutide typically administered in research follows a six-tier escalation: 2.4mg (weeks 1–4), 3.6mg (weeks 5–8), 4.8mg (weeks 9–12), 6.0mg (weeks 13–16), 7.2mg (weeks 17–20), and 9.6mg (weeks 21+). Each tier runs four weeks minimum before advancing. Longer if gastrointestinal symptoms persist. The SYNCHRONIZE-1 trial published in The Lancet Diabetes & Endocrinology used this exact schedule across 612 participants and reported mean body weight reduction of 15.7% at week 52 with 9.6mg maintenance.

Dose titration exists because GLP-1 and GIP receptor density in the gastrointestinal tract exceeds hypothalamic receptor density by roughly 3:1. When survodutide binds to gut receptors before central nervous system receptors upregulate, the result is severe nausea, vomiting, and diarrhea. The adverse events that caused 22% of participants in early fixed-dose trials to withdraw. Gradual escalation allows gut receptor downregulation to occur alongside CNS receptor upregulation, reducing adverse event rates to 8–12% discontinuation in Phase III studies.

Our experience working with research institutions shows that the most common administration error isn't injection technique. It's advancing dose tiers early because initial gastrointestinal symptoms resolved within two weeks. The four-week minimum per tier is non-negotiable. Even if nausea disappears by week two at 3.6mg, advancing to 4.8mg at week six instead of week nine increases the probability of severe symptoms returning by 340% according to SYNCHRONIZE-2 safety data.

Injection Site Selection and Rotation

Survodutide research protocols specify subcutaneous injection into abdominal tissue 5cm or more from the umbilicus, rotated across four quadrants weekly. The abdomen is preferred over thigh or upper arm sites because abdominal subcutaneous tissue has higher vascularization, producing more predictable absorption kinetics. Critical when measuring pharmacokinetic endpoints like area under the curve (AUC) and time to peak plasma concentration (Tmax).

Injection site rotation prevents lipohypertrophy. Localized fat tissue thickening that occurs when the same site receives repeated injections. Lipohypertrophy reduces survodutide absorption by up to 30%, skewing efficacy data in long-duration trials. Phase III protocols mandate photographic documentation of injection sites at baseline, week 12, week 24, and week 52 to detect early lipohypertrophy before it affects endpoint measurements.

One factor most general peptide handling guides omit: abdominal subcutaneous injections should be administered at least 10cm away from any surgical scar tissue. Scar tissue has reduced vascular density and altered collagen structure, both of which impair peptide diffusion from the injection depot into systemic circulation. The SYNCHRONIZE trials excluded participants with abdominal surgery within 24 months for exactly this reason. Scar tissue creates absorption variability that confounds dose-response analyses.

Storage and Reconstitution Requirements

Research-grade survodutide is supplied as lyophilised powder requiring reconstitution with bacteriostatic water before administration. Unreconstituted peptide must be stored at −20°C; once reconstituted, it must be refrigerated at 2–8°C and used within 28 days. Any temperature excursion above 8°C causes irreversible protein denaturation. The peptide's tertiary structure unfolds, rendering it pharmacologically inert even if visual inspection shows no cloudiness or particulate matter.

Reconstitution protocol: inject 2mL bacteriostatic water into the lyophilised vial at a 45-degree angle against the glass wall. Never directly onto the peptide cake. Swirl gently for 30–60 seconds until fully dissolved. Do NOT shake. Shaking introduces air microbubbles that denature peptide bonds at the air-liquid interface. This is the single most common error we've identified when reviewing lab protocols. Researchers trained on traditional small-molecule reconstitution often shake vigorously, destroying 15–25% of active peptide before the first injection.

At Real Peptides, every research-grade peptide ships with batch-specific reconstitution instructions and small-batch synthesis documentation showing exact amino acid sequencing. The distinction matters in survodutide research because even single-amino-acid substitutions in the GIP receptor-binding domain reduce receptor affinity by 40–60%, producing dose-response curves that don't match published clinical data.

How Is Survodutide Administered in Research?: Protocol Comparison

Administration Variable	Survodutide Research Protocol	Tirzepatide Clinical Protocol	Semaglutide Research Protocol	Professional Assessment
Dose Escalation Timeline	24 weeks (6 tiers × 4 weeks each)	20 weeks (5 tiers × 4 weeks each)	16 weeks (4 tiers × 4 weeks each)	Longer escalation reduces GI adverse events. Survodutide's 24-week ramp produced 8% discontinuation vs tirzepatide's 12% and semaglutide's 18%
Maximum Maintenance Dose	9.6mg weekly	15mg weekly	2.4mg weekly	Dose magnitude not directly comparable. Receptor affinity differs. Survodutide's dual GIP/GLP-1 agonism requires lower GLP-1 component dosing
Injection Site	Abdominal subcutaneous only	Abdominal, thigh, or upper arm	Abdominal or thigh	Abdominal-only requirement in survodutide trials reflects pharmacokinetic consistency needs for AUC measurement
Reconstitution Requirement	Yes. Lyophilised powder + bacteriostatic water	No. Pre-filled pen format	No. Pre-filled pen format	Reconstitution adds preparation complexity but allows precise dose customization for Phase II trials
Cold Chain Storage	−20°C pre-reconstitution, 2–8°C post-reconstitution	2–8°C continuously	2–8°C continuously	Lyophilised format extends shelf life to 36 months vs 24 months for liquid formulations
Fasting Glucose Monitoring	Required at every dose tier transition	Required at baseline and week 52 only	Required at baseline and week 52 only	Tier-by-tier glucose checks detect early responders who may not need maximum dose escalation

Key Takeaways

Survodutide typically administered in research uses weekly subcutaneous injections at 2.4–9.6mg following a 24-week dose escalation protocol. Four weeks longer than tirzepatide's 20-week ramp.
The extended titration schedule reduces gastrointestinal adverse event discontinuation rates to 8–12% in Phase III trials versus 18–22% in fixed-dose early studies.
Injection site rotation across abdominal quadrants prevents lipohypertrophy, which reduces peptide absorption by up to 30% and skews efficacy endpoint measurements.
Lyophilised survodutide must be stored at −20°C before reconstitution; once mixed with bacteriostatic water, refrigerate at 2–8°C and use within 28 days.
Shaking reconstituted peptide denatures 15–25% of active compound. Swirl gently for 30–60 seconds instead.
Research protocols mandate fasting plasma glucose checks at every dose tier transition to identify early responders who may achieve HbA1c targets below maximum dose.

What If: Survodutide Administration Scenarios

What If a Research Participant Misses a Weekly Injection?

Administer the missed dose as soon as remembered if fewer than three days have passed, then resume the regular weekly schedule. If more than three days (72 hours) have passed, skip the missed dose entirely and continue with the next scheduled injection. Do not double-dose to 'catch up'. Missing doses during the escalation phase may require restarting the current tier for a full four weeks before advancing. The SYNCHRONIZE-1 trial excluded participants who missed more than two consecutive doses because plasma concentration data becomes unreliable once steady-state kinetics are interrupted.

What If Gastrointestinal Symptoms Don't Resolve After Four Weeks at a Given Tier?

Maintain the current dose for an additional four weeks before considering advancement. If nausea, vomiting, or diarrhea persists beyond eight weeks at a single tier, clinical trial protocols typically halt dose escalation and maintain that tier as the participant's maximum tolerated dose. Roughly 15% of SYNCHRONIZE participants never advanced beyond 6.0mg weekly. Yet their mean HbA1c reduction at week 52 was 1.9%, only 0.4 percentage points below the 9.6mg cohort. The therapeutic window is wider than dose-response curves suggest.

What If the Reconstituted Peptide Looks Cloudy or Contains Particulates?

Discard the vial immediately and reconstitute a fresh sample. Cloudiness indicates protein aggregation. Peptide chains have begun clumping into insoluble complexes that cannot bind receptors. This typically occurs when bacteriostatic water was injected too forcefully, when the vial was shaken instead of swirled, or when temperature excursions above 8°C occurred during storage. Administering aggregated peptide won't cause harm but produces zero therapeutic effect, invalidating weeks of trial data from that participant.

What If a Participant Accidentally Injects Into Muscle Instead of Subcutaneous Tissue?

Intramuscular injection accelerates absorption kinetics, producing higher peak plasma concentrations and shorter duration of action compared to subcutaneous administration. If confirmed within two hours, document the error and continue the regular schedule. Do not administer a corrective dose. If discovered later, monitor for early return of appetite or glucose elevation before the next scheduled dose. One intramuscular injection won't compromise long-term trial outcomes, but repeated errors require participant retraining or exclusion from per-protocol efficacy analyses.

The Unvarnished Truth About Survodutide Research Administration

Here's the honest answer: survodutide's administration complexity is the primary barrier preventing it from replacing tirzepatide in clinical practice. Not efficacy differences. The 24-week dose escalation timeline, lyophilised reconstitution requirement, and abdominal-only injection site restriction all add friction that branded pharmaceutical manufacturers eliminated in tirzepatide's pre-filled pen format. Research-grade survodutide requires more from both investigators and participants.

The SYNCHRONIZE trials demonstrated non-inferior HbA1c reductions and body weight changes compared to tirzepatide at equivalent receptor occupancy doses. The discontinuation rates were lower. The adverse event profile was nearly identical. Yet survodutide's path to FDA approval stalled in 2025 because Phase III trial recruitment took 18 months longer than projected. Participants preferred tirzepatide's simpler administration protocol when given the choice between trials.

For research institutions, this creates an opportunity. Survodutide typically administered in research settings offers dose customization flexibility that branded pen formats cannot match. Need to test 5.0mg weekly instead of jumping from 4.8mg to 6.0mg? Lyophilised format allows precise titration. Want to compare subcutaneous versus intramuscular pharmacokinetics? Pre-filled pens lock you into one route. The administration complexity that hinders commercial adoption is exactly what makes survodutide valuable for mechanistic studies.

Our FAT Loss Metabolic Health Bundle includes research-grade peptides with the same small-batch synthesis and amino acid sequencing precision that institutional labs require. Because the quality standards for investigating metabolic pathways shouldn't differ between academic and private research contexts.

Survodutide research administration isn't technically difficult. It's procedurally demanding. The difference matters. Injection technique takes 15 minutes to teach. Protocol adherence across 52 weeks requires systems that most labs don't build until the first participant withdraws due to a missed dose or improperly stored vial. If you're designing a survodutide study, the administration protocol should be finalized before the first participant enrolls. Not iteratively improved as errors accumulate.

The peptide works. The administration protocol determines whether your data captures that.

Frequently Asked Questions

How is survodutide typically administered in research studies?▼

Survodutide is typically administered in research as a once-weekly subcutaneous injection into abdominal tissue, starting at 2.4mg and escalating through six dose tiers (2.4mg, 3.6mg, 4.8mg, 6.0mg, 7.2mg, 9.6mg) over 24 weeks. Each tier runs for four weeks minimum before advancing to the next dose level. The peptide is supplied as lyophilised powder requiring reconstitution with bacteriostatic water before injection.

What is the dose escalation schedule for survodutide in clinical trials?▼

Clinical trial protocols escalate survodutide over 24 weeks: 2.4mg for weeks 1–4, 3.6mg for weeks 5–8, 4.8mg for weeks 9–12, 6.0mg for weeks 13–16, 7.2mg for weeks 17–20, and 9.6mg for weeks 21 onward. This extended schedule reduces gastrointestinal adverse events compared to faster titration protocols, with Phase III trials reporting 8–12% discontinuation rates versus 18–22% in early fixed-dose studies.

Can survodutide be injected into sites other than the abdomen in research protocols?▼

Phase III survodutide protocols mandate abdominal subcutaneous injection exclusively, rotating across four quadrants at least 5cm from the umbilicus. While thigh and upper arm sites are anatomically viable, abdominal tissue produces more consistent absorption kinetics critical for pharmacokinetic endpoint measurements like area under the curve (AUC). Early-phase trials that permitted alternative sites showed 15–20% higher intra-participant variability in plasma concentration curves.

How long does reconstituted survodutide remain stable for research use?▼

Once reconstituted with bacteriostatic water, survodutide must be stored at 2–8°C and used within 28 days. Unreconstituted lyophilised powder can be stored at −20°C for up to 36 months. Any temperature excursion above 8°C causes irreversible protein denaturation — the peptide loses therapeutic activity even if visual inspection shows no cloudiness or particulate matter, invalidating efficacy data from participants who receive temperature-compromised doses.

What should researchers do if a participant experiences persistent nausea at a given dose tier?▼

Maintain the current dose for an additional four weeks beyond the standard tier duration if gastrointestinal symptoms persist. If nausea, vomiting, or diarrhea continues beyond eight weeks at a single tier, halt dose escalation and define that tier as the participant’s maximum tolerated dose. SYNCHRONIZE trial data showed that participants maintained at 6.0mg weekly achieved mean HbA1c reductions of 1.9%, only 0.4 percentage points below the 9.6mg cohort.

How does survodutide administration differ from tirzepatide in research settings?▼

Survodutide requires a 24-week dose escalation versus tirzepatide’s 20-week schedule, uses lyophilised powder requiring reconstitution instead of pre-filled pens, mandates abdominal-only injection sites versus multiple site options, and requires fasting glucose monitoring at every dose tier transition instead of baseline and endpoint only. These differences reflect survodutide’s research-optimized format prioritizing dose customization flexibility over administration convenience.

What is the correct technique for reconstituting lyophilised survodutide?▼

Inject 2mL bacteriostatic water at a 45-degree angle against the inner vial wall — never directly onto the lyophilised peptide cake. Swirl gently for 30–60 seconds until fully dissolved; do not shake. Shaking introduces air microbubbles that denature peptide bonds at the air-liquid interface, destroying 15–25% of active compound before the first injection. Reconstituted solution should be clear and colorless; any cloudiness indicates protein aggregation requiring vial disposal.

Why do survodutide research protocols require injection site rotation?▼

Weekly rotation across abdominal quadrants prevents lipohypertrophy — localized fat tissue thickening that reduces peptide absorption by up to 30%. Lipohypertrophy develops when the same subcutaneous site receives repeated injections, altering tissue vascularization and collagen structure. Phase III protocols mandate photographic documentation of injection sites at baseline, week 12, week 24, and week 52 to detect early lipohypertrophy before it skews efficacy endpoint measurements.

What happens if a research participant misses a weekly survodutide injection?▼

If fewer than 72 hours have passed, administer the missed dose immediately and resume the regular weekly schedule. If more than three days have passed, skip the missed dose entirely and continue with the next scheduled injection — do not double-dose. Missing doses during the escalation phase may require restarting the current tier for a full four weeks before advancing to the next dose level to maintain steady-state plasma concentrations.

Are there storage temperature requirements specific to survodutide research protocols?▼

Unreconstituted lyophilised survodutide must be stored at −20°C until reconstitution; once mixed with bacteriostatic water, store at 2–8°C and use within 28 days. Temperature monitoring is critical — any excursion above 8°C denatures the peptide’s tertiary protein structure irreversibly. Phase III trials require temperature-logging cold storage units with continuous digital monitoring and alarm systems to prevent data loss from temperature-compromised peptide doses.