Cerebrolysin

What it is

Cerebrolysin is a neurotrophic peptide preparation — and the “preparation” word matters, because unlike most entries in this wiki it isn’t one defined molecule. Per peptidelist, it is “a mixture of peptides and amino acids derived from pig brain tissue, researched extensively for neurotrophic and neuroprotective effects, particularly in cognitive recovery”. The manufacturer, EVER Neuro Pharma (Austria), produces it by enzymatic breakdown of purified porcine brain protein into a standardized blend of low-molecular-weight peptides (<10 kDa) and free amino acids designed to mimic the body’s own neurotrophic factors [0035; peptidelist].

That porcine-brain origin is also its defining practical feature: it’s administered by intravenous or intramuscular infusion in a clinical setting — not the at-home subcutaneous injection model of most research peptides. This is a drug with a 40-year prescribing history in much of the world, not a gray-market biohacking compound, even though in the US it sits in research-only status.

How it works

Per peptidelist, Cerebrolysin “contains neurotrophic factors that may support neuronal survival, synaptic plasticity, and neurogenesis”. The mechanistic claim is that its peptide fraction acts like the brain’s endogenous neurotrophic signaling — the same family of “keep neurons alive and growing” signals that Semax and Selank upregulate indirectly via BDNF/NGF. Three proposed channels [0035; peptidelist]:

• Neuronal survival / neuroprotection — protecting neurons from ischemic and excitotoxic death, the rationale for its use in the acute window after a stroke.
• Synaptic plasticity — supporting the formation and remodeling of synaptic connections, the basis for the cognitive-recovery and dementia indications.
• Neurogenesis — supporting the generation of new neurons.

The honest caveat: because Cerebrolysin is a mixture rather than a single molecule, its mechanism is characterized at the level of “neurotrophic-factor-mimetic effects” rather than a clean single-receptor story. That’s a real difference from the rest of this wiki’s cognitive peptides, and it’s part of why Western reviewers grade the evidence cautiously even though the clinical-use history is long.

What the research shows

This is the unusual part: Cerebrolysin has more human data than almost any peptide in this wiki, and yet the Western quality verdict is mixed. Both facts deserve full weight.

The scale of the human record. Peptidelist grades it Strong: 30 studies cited, 19 human trials, Phase 3 reached. Its own evidence summary states the body comprises 29 human studies including 4 RCTs. By the raw count of human trials, this is a heavily-studied compound — the opposite of the animal-only profile common to bleeding-edge peptides.

What the trials actually found [all per KB doctrine on third-party citations]:

Study	Year	Type / n	Finding
Muresanu DF et al. — CARS trial, Stroke ( 26564102)	2016	, 90-day	Cerebrolysin significantly improved upper-extremity motor function at day 90 post-stroke vs. placebo
Alvarez XA et al. — Eur J Neurol ( 20500802)	2011	, n=133, 12 wk	At all three dosages, improved global clinical function and cognition in moderate-to-moderately-severe Alzheimer’s
Khasanova DR, Kalinin MN — CEREHETIS pilot ( 37682097)	2023	, n=341	With alteplase, reduced symptomatic hemorrhagic transformation — but no functional benefit at 90 days
Kalinin MN, Khasanova DR — CEREHETIS post-hoc ( 40123141)	2025	, n=238	Reduced hemorrhagic-transformation risk; enabled earlier anticoagulation resumption

So on the positive side: a placebo-controlled Phase 3-grade stroke trial (CARS) showing a real motor-recovery signal, and a double-blind Alzheimer’s RCT showing cognitive and global-function improvement. That’s a stronger positive human signal than most peptides in this KB can claim.

The Cochrane caveat — stated honestly. The Cochrane reviews of Cerebrolysin for acute ischemic stroke are the central Western quality verdict, and they are not flattering [all]:

• Ziganshina LE et al. 2023 Cochrane Database Syst Rev ( 37818733, n=1773): Cerebrolysin shows no benefit on mortality in acute ischemic stroke, with a potential increase in non-fatal serious adverse events.
• Ziganshina LE et al. 2020 ( 32662068, n=1601) and 2017 ( 28430363, n=1501): same conclusion — little or no clinical benefit for acute ischemic stroke, with a potential increase in non-fatal serious adverse events.

Peptidelist’s own integrated summary captures the split precisely: “Among 30 studies (29 human, 4 RCTs), cerebrolysin showed mixed efficacy: it reduced symptomatic hemorrhagic transformation when combined with alteplase in acute stroke but provided no functional benefit at 90 days, and while it improved cognition and global function in vascular dementia, the evidence quality was rated very low; additionally, cerebrolysin demonstrated no mortality benefit in acute ischemic stroke and raised concerns for increased non-fatal serious adverse events”.

The honest synthesis. Two readings coexist, and OHM reports both:

• The established-clinical-use reading: Cerebrolysin has a 40-year European/Asian prescribing record, a positive Phase 3 stroke motor-recovery trial (CARS), and a positive Alzheimer’s RCT (Alvarez). For vascular dementia and stroke rehabilitation it is genuinely a standard-of-care option across much of the world.
• The Western evidence-quality reading: Cochrane rates the acute-stroke evidence “very low quality,” finds no mortality benefit, and flags a non-fatal serious-AE signal. Where the trials are positive (motor function, dementia cognition), the methodological grade is weak by Western RCT standards.

Neither erases the other. 0035 landed it at Tier B (not A) precisely because of this split — “mixed efficacy + Cochrane quality grade + serious-AE concern… The Ph3 data exists but it isn’t a clean A”.

The hemorrhagic-SAE signal — surfaced, not buried

The one safety item that deserves its own section, because it’s specific and it’s real:

In the CEREHETIS trials, Cerebrolysin was given combined with alteplase (the clot-busting thrombolytic) in acute stroke. The headline finding was actually protective — it reduced symptomatic hemorrhagic transformation (bleeding into the infarcted brain tissue, a feared complication of thrombolysis) — but it produced no functional benefit at 90 days in that readout [peptidelist; 0035, PMID 37682097]. Separately, the Cochrane reviews flag a potential increase in non-fatal serious adverse events in acute ischemic stroke generally, and network meta-analyses rated other neuroprotective agents (NBP, edaravone, edaravone dexborneol) as safer/more effective for acute stroke outcomes [peptidelist, PMIDs 37818733, 39575393, 39834702].

The honest read: the hemorrhagic-transformation data is mixed in direction (reduced bleeding in the alteplase combo, but a general non-fatal-SAE signal across the Cochrane pool) and concentrated in the acute-stroke-plus-thrombolytic setting — a hospital-managed scenario, not the elective-cognitive-enhancement use case. But it’s a documented signal, it’s why 0035 set the safety light to yellow, and an encyclopedia that aspires to be the credible source names it rather than reciting only the positive Alzheimer’s and motor-recovery results.

Real-world protocol

The information here is educational only. Cerebrolysin is administered by IV/IM infusion and is not FDA-approved in the US. This is not medical advice; the established protocols below are administered clinically in the countries where the drug is approved.

Cerebrolysin is not a self-inject SubQ peptide — the established route is IV or IM infusion in a clinical setting, which is part of why it sits apart from the rest of this wiki’s at-home cognitive peptides. The clinical protocols documented in the countries where it’s approved (broadly, from the EVER Neuro Pharma labeling and the trial designs above) run as daily IV infusions over a 10–20 day course, repeated as cycles — the CARS and Alvarez trial structures reflect this multi-week course model rather than a continuous-dosing model [peptidelist; trial designs]. Specific dose-per-infusion and concentration vary by indication and are set clinically.

Because the established use is infusion-based and physician-administered in approving jurisdictions, there isn’t a “community insulin-syringe protocol” to report the way there is for self-inject peptides like BPC-157 or Semax. The honest statement is: the documented protocol is the clinical IV/IM course, not a DIY SubQ regimen.

Side effects & management

The clinical-trial AE profile is generally mild at standard infusion dosing, with the specific signals noted above [peptidelist; 0035]:

• Infusion-related effects — the most common practical issue with IV/IM administration; managed by infusion-rate control in clinical settings.
• Allergy / hypersensitivity — because Cerebrolysin is a porcine-brain-derived biological mixture, allergic/hypersensitivity reactions are a recognized concern and part of why 0035 set the safety light to yellow (“IV admin + allergy + the SAE signal”).
• The non-fatal serious-AE signal in the acute-stroke Cochrane pool, and the hemorrhagic-transformation considerations in the alteplase-combination setting, detailed above.

Contraindications in standard clinical use include hypersensitivity to the product and (per labeling in approving countries) certain epileptic and severe-renal contexts.

Regulatory status

Cerebrolysin is approved and marketed across much of Europe, Asia, Russia, and Latin America, where it has a 40-year prescribing history for stroke, dementia, and TBI. In the United States it is NOT FDA-approved and is sold/handled as a research compound; peptidelist lists its US availability as “mixed” (some compounding-pharmacy and research-supplier access) and its formal status as research-only. WADA status is not a primary concern for this neurology compound. Factual, no editorializing: established prescription drug abroad, unapproved research compound in the US.

The Alyve product

Cerebrolysin is not in Alyve’s launch catalog. It’s a porcine-brain-derived, infusion-administered biological — a different category from the at-home research peptides Alyve carries — so this is an encyclopedia/authority entry, not a CTA target. There’s no fabricated offer here; Alyve doesn’t sell it.

For a reader who arrived looking at the cognitive / neuroprotection goal Cerebrolysin addresses, the in-catalog and KB-covered options are the self-inject cognitive peptides with cleaner single-molecule mechanisms and at-home protocols:

• Semax and Selank — the strongest-evidenced Russian nootropic peptides (acute, receptor-mediated BDNF/NGF upregulation), covered in full in their standalone articles.
• The broader cognitive cluster — Cognitive peptides cluster — Dihexa, Pinealon, Cortagen (Dihexa, Pinealon, Cortagen) for the bleeding-edge end.
• Glutathione for the foundational antioxidant layer.

The supply-chain trust story still frames the category honestly: roughly a quarter of gray-market peptide supply tests fake or underdosed, and for any neuro-active compound, identity and purity verification is the floor. For the in-catalog cognitive SKUs, Alyve’s positioning is US-manufactured + third-party Freedom Diagnostics COAs + >99% verified purity across the board.

Offer (for the in-catalog cognitive options, not Cerebrolysin): Use coupon OHM-15 for 15% off — Alyve’s pricing is very competitive, and buying 3 vials of any given peptide in one purchase gets you over 30% off retail. (Full disclosure: OHM-15 attributes the sale to me — said plainly, as always.)

Sources

1. — thepeptidelist.com profile: porcine-brain peptide mixture (EVER Neuro Pharma), 30 studies / 29 human / 4 RCTs / Phase 3, the integrated mixed-efficacy evidence summary, named RCT + Cochrane PMIDs (all), mixed US availability / research-only status.
2. (lines 78–89) — Tier B / Safety Yellow / grading; the “why B not A” (mixed efficacy + Cochrane quality + SAE concern) and “why yellow” (IV admin + allergy + SAE signal) rationale; the OHM funcmed-lean editorial note (“long-standing European/Asian clinical-practice peptide… capture both sides honestly”); the open-VERIFY note on whether to upgrade from B/yellow (line 692).
3. Cerebrolysin named anchors (all): Muresanu CARS 2016 26564102; Alvarez 2011 20500802; Khasanova CEREHETIS 2023 37682097; Kalinin CEREHETIS post-hoc 2025 40123141; Ziganshina Cochrane 2023 37818733 / 2020 32662068 / 2017 28430363.

Related: Semax · Selank · Cognitive peptides cluster — Dihexa, Pinealon, Cortagen · Glutathione · BPC-157.