What is the best peptide tracking app?

DoseCraft is the most comprehensive peptide tracking app — 90+ compounds with evidence tiers, half-life-aware scheduling, built-in reconstitution calculator, injection-site rotation, and 6 AI coaches. Free tier available; Pro is $59.99/year with a 7-day free trial, or $149.99 Founder Lifetime for the first 1,000 users.

Is DoseCraft a ChatGPT wrapper?

No. DoseCraft's AI is trained on a proprietary corpus of 10,000+ hours of curated peptide-practitioner expertise — protocol audits, bloodwork reviews, cycle logs, interaction matrices — that is not in any general LLM's training set. Every answer comes from expert-reviewed material, not recycled public-web content.

Does DoseCraft work on iPhone?

Yes. DoseCraft is available on iOS 17+ on the Apple App Store. Android and Apple Watch support are on the roadmap.

DoseCraft has a free tier with basic logging and library browsing. Pro ($59.99/year with 7-day trial, $9.99/month, or $149.99 Founder Lifetime) unlocks unlimited protocols, all 6 AI coaches, interaction alerts, outcome correlation, CSV and PDF export.

Can DoseCraft calculate peptide reconstitution?

Yes. DoseCraft has a built-in reconstitution calculator that computes BAC water volume, units-per-draw on insulin syringes, and vial shelf life across every compound in the library.

Is DoseCraft medical advice?

No. DoseCraft is a research and tracking tool. Peptides referenced are sold 'for research use only' by third-party suppliers. DoseCraft does not sell peptides, does not prescribe, and does not constitute medical advice. Always consult a licensed physician.

Can I delete my DoseCraft account?

Yes. Profile → Delete Account performs an irreversible wipe of your account and all associated data. Available in-app and via dosecraftapp.com/delete-account. Apple 5.1.1(v) compliant.

All comparisons

GLP-1

Semaglutide vs Liraglutide

TL;DR

Liraglutide is the first-generation GLP-1 receptor agonist — daily injection, ~13-hour half-life. Semaglutide is the second-generation version — weekly injection, ~7-day half-life, stronger magnitude on weight and HbA1c endpoints. The research question is rarely which to pick, it's why someone would still pick Liraglutide.

VerdictSema edges

Semaglutide beats Liraglutide on every meaningful axis for modern research: half-life (~7 days vs ~13 hours), magnitude of effect, and dosing cadence. Liraglutide is the first-generation tool that Semaglutide was designed to improve on. There's rarely a protocol reason to choose Liraglutide today except supply-constraint scenarios.

Contender A

Semaglutide

Also: Sema

Mechanism

Long-acting GLP-1 receptor agonist — fatty-acid modification extends half-life to weekly dosing. Same receptor, same class, different kinetics.

Half-life: ~7 days
Primary use: Modern GLP-1 research
Dose range: 0.25 mg -> 2.4 mg weekly
Cost tier: $$ · Moderate sourcing cost

Clinical evidence tier

Contender B

Liraglutide

Also: Lira

Mechanism

First-generation GLP-1 receptor agonist — shorter fatty-acid chain, daily dosing, same receptor pharmacology as Semaglutide.

Half-life: ~13 hours
Primary use: Legacy GLP-1 research
Dose range: 0.6 mg -> 3.0 mg daily
Cost tier: $$ · Moderate sourcing cost

Clinical evidence tier

Detailed Comparison

10 attributes side-by-side. Highlighted rows show where one tool has a clear structural edge.

Attribute	Sema	Lira	Edge
Receptor target	GLP-1	GLP-1	Tie
Half-life	~7 days	~13 hours	Sema
Dosing cadence	Weekly	Daily	Sema
Weight-change magnitude	~15% in 68 weeks	~8% in 56 weeks	Sema
HbA1c reduction	~1.8%	~1.2%	Sema
GI tolerability	Moderate ramp	Similar ramp, more daily exposure	Sema
Pulsatile vs steady GLP-1 signaling	Steady (weekly)	Peak-and-trough (daily)	Sema
Evidence maturity	Very mature	Most mature (earliest)	Lira
Research-sourcing cost	Moderate	Similar	Tie
Protocol simplicity	Simple (weekly)	Disciplined (daily)	Sema

Deep dive

Full Semaglutide research profile

Deep dive

Full Liraglutide research profile

Practitioner Notes

Sourced from DoseCraft's 10,000+ hour practitioner corpus — not PubMed abstracts.

Liraglutide was the first GLP-1 agonist to show meaningful weight-loss magnitude and it still has real use in legacy research — protocols where the daily dosing pattern is specifically needed (sensitivity studies, fine-grained titration) or where Liraglutide has the longer clinical-data history that a research question demands.

For every other modern protocol, Semaglutide is structurally better. The ~7-day half-life and weekly dosing produce fewer protocol-adherence failures, and the magnitude of effect on both weight and HbA1c is roughly 50-70% larger than Liraglutide at comparable receptor saturation.

In the practitioner corpus we reference, the one consistent scenario where Liraglutide still appears: research subjects with extreme GI sensitivity who cannot tolerate the higher integrated exposure of weekly Semaglutide. The daily peak-and-trough pattern of Liraglutide is actually gentler in rare cases. This is a narrow slice of protocols.

Stacking & Switching

Can these be combined? Should you switch from one to the other? Titration considerations.

Stack compatibility: See the “Stacks well” or “Stack compatibility” row in the comparison table above. When the edge column shows Tie, both compounds run together cleanly. When one compound dominates, check the protocol notes for the specific stacking pattern practitioners use.

Switching protocol: The general pattern across practitioner protocols: hold the current dose stable, introduce the new compound at its lowest titration step, run both for a 1-2 week cross-over window, then taper the original. Abrupt switches produce rebound effects as the original compound's steady state clears.

Half-life math: DoseCraft's PK-aware AI models half-life decay and stack overlap across every pairing above. The 20x20 interaction matrix flags contraindications automatically — no manual math, no overlapping-signal blindspots.

Frequently Asked Questions

Indexed for SERP FAQPage rich results.

Is Liraglutide just a weaker Semaglutide?

Effectively yes. Same receptor, same class, shorter half-life, smaller magnitude. Semaglutide was engineered as the improved version of Liraglutide.

Why would anyone still use Liraglutide?

Legacy clinical-data comparability, daily-titration sensitivity protocols, or rare GI-tolerance edge cases where the peak-and-trough pattern is easier than weekly steady state.

Can I switch from Liraglutide to Semaglutide?

Yes. Most practitioner protocols hold the Liraglutide dose, introduce Semaglutide at 0.25 mg weekly, run both for 1 week, then discontinue Liraglutide. Abrupt switches produce a brief appetite rebound as the daily peak clears.

Are side effects similar?

Same class of side effects (nausea, constipation, occasional pancreatitis signals in outliers). Magnitude tracks integrated exposure — weekly Sema at steady state produces more continuous exposure than daily Lira does across the day.

What about Tirzepatide in this conversation?

Tirzepatide is the dual-pathway successor — GIP + GLP-1 vs Semaglutide's GLP-1 only. See our Semaglutide vs Tirzepatide comparison for the current generational tradeoff.

Related Comparisons

GLP-1

Semaglutide vs Tirzepatide

Semaglutide is a single-pathway GLP-1 receptor agonist with ~7-day half-life. Tirzepatide is a dual GIP and GLP-1 agonist with ~5-day half-life and meaningfully larger magnitude on both weight and HbA1c endpoints. Both are weekly-administered research peptides; the tradeoff is potency vs tolerability and cost.

Read

GLP-1

Tirzepatide vs Retatrutide

Tirzepatide is a dual GIP / GLP-1 agonist with mature clinical data. Retatrutide is a triple agonist adding glucagon receptor activation, producing larger weight-loss signals in Phase 2 research but with less long-term safety data and a steeper side-effect curve.

Read

Longevity

MOTS-c vs SS-31

MOTS-c is a mitochondrial-derived peptide that signals systemically — it activates AMPK, improves insulin sensitivity, and enhances exercise capacity. SS-31 (elamipretide) is a mitochondrial-targeting peptide that binds cardiolipin on the inner mitochondrial membrane, preserving electron-transport-chain function and reducing oxidative damage. Same organelle, completely different mechanism.

Read

Track Your Protocol with PK-Aware AI

Compound choice is step one. DoseCraft models half-life decay, stack overlap, and titration paths across 90+ peptides — the only peptide tool with a real pharmacokinetic reasoning layer on top of a 10,000+ hour practitioner corpus.

Track your protocol with PK-aware AI in DoseCraft

Research-only disclaimer: This comparison is for research and educational purposes only. Peptides referenced are sold for research use by third-party suppliers. Not evaluated by the FDA. Not intended to diagnose, treat, cure, or prevent any disease. Always consult a licensed physician before acting on any peptide protocol information.

Semaglutide vs Liraglutide

TL;DR

VerdictSema edges

Attribute

Sema

Lira

Edge

Receptor target

GLP-1

Tie

Half-life

~7 days

~13 hours

Sema

Dosing cadence

Weekly

Daily

Sema

Weight-change magnitude

~15% in 68 weeks

~8% in 56 weeks

Sema

HbA1c reduction

~1.8%

~1.2%

Sema

GI tolerability

Moderate ramp

Similar ramp, more daily exposure

Sema

Pulsatile vs steady GLP-1 signaling

Steady (weekly)

Peak-and-trough (daily)

Sema

Evidence maturity

Very mature

Most mature (earliest)

Lira

Research-sourcing cost

Moderate

Similar

Tie

Protocol simplicity

Simple (weekly)

Disciplined (daily)

Sema