Curcumin for Neurodegeneration
<table class="infobox infobox-therapeutic">
<tr>
<th class="infobox-header" colspan="2">Curcumin for Neurodegeneration</th>
</tr>
<tr>
<td class="label">Dimension</td>
<td>Score</td>
</tr>
<tr>
<td class="label">Mechanistic Clarity</td>
<td>7/10</td>
</tr>
<tr>
<td class="label">Clinical Evidence</td>
<td>3/10</td>
</tr>
<tr>
<td class="label">Preclinical Evidence</td>
<td>7/10</td>
</tr>
<tr>
<td class="label">Replication</td>
<td>4/10</td>
</tr>
<tr>
<td class="label">Effect Size</td>
<td>3/10</td>
</tr>
<tr>
<td class="label">Safety/Tolerability</td>
<td>9/10</td>
</tr>
<tr>
<td class="label">Biological Plausibility</td>
<td>5/10</td>
</tr>
<tr>
<td class="label">Actionability</td>
<td>2/10</td>
</tr>
<tr>
<td class="label">Formulation</td>
<td>Technology</td>
</tr>
<tr>
<td class="label">Longvida SLCP</td>
<td>Solid Lipid Curcumin Particle; lecithin-lipid matrix</td>
</tr>
<tr>
<td class="label">Theracurmin</td>
<td>Nanoparticle colloidal suspension (180nm)</td>
</tr>
<tr>
<td class="label">Meriva (Phytosome)</td>
<td>Phosphatidylcholine complexation</td>
</tr>
<tr>
<td class="label">BCM-95/Biocurcumax</td>
<td>Curcumin + essential oils + piperine</td>
</tr>
<tr>
<td class="label">C3 Complex + Piperine</td>
<td>Standard extract + BioPerine (5mg piperine)</td>
</tr>
<tr>
<td class="label">NovaSOL</td>
<td>Micelle (polysorbate 80)</td>
</tr>
<tr>
<td class="label">Factor</td>
<td>Consideration</td>
</tr>
<tr>
<td class="label">Formulation choice</td>
<td>Longvida SLCP preferred for CNS targeting; Theracurmin acceptable</td>
</tr>
<tr>
<td class="label">Dysphagia</td>
<td>Capsule contents can be mixed with food; liquid Theracurmin available</td>
</tr>
<tr>
<td class="label">Disease stage</td>
<td>Earlier intervention preferred; brain curcumin levels unlikely to halt advanced neurodegeneration</td>
</tr>
<tr>
<td class="label">Monitoring</td>
<td>No established biomarkers; plasma curcumin levels poorly correlated with brain exposure</td>
</tr>
<tr>
<td class="label">Realistic expectations</td>
<td>Anti-inflammatory and antioxidant support rather than disease modification; manage patient expectations accordingly</td>
</tr>
<tr>
<td class="label">Population</td>
<td>Formulation</td>
</tr>
<tr>
<td class="label">Prevention (healthy elderly)</td>
<td>Longvida SLCP</td>
</tr>
<tr>
<td class="label">MCI / early cognitive decline</td>
<td>Theracurmin or Longvida</td>
</tr>
<tr>
<td class="label">Active AD/PD</td>
<td>Longvida SLCP</td>
</tr>
<tr>
<td class="label">PSP/CBS</td>
<td>Longvida SLCP</td>
</tr>
<tr>
<td class="label">Depression comorbidity</td>
<td>BCM-95</td>
</tr>
<tr>
<td class="label">Medication</td>
<td>Interaction</td>
</tr>
<tr>
<td class="label">Warfarin/DOACs</td>
<td>Mild additive anticoagulation</td>
</tr>
<tr>
<td class="label">Tamoxifen</td>
<td>May reduce efficacy via UGT induction</td>
</tr>
<tr>
<td class="label">Piperine-sensitized formulations + CYP substrates</td>
<td>Piperine inhibits CYP3A4, CYP2D6</td>
</tr>
<tr>
<td class="label">Levodopa</td>
<td>No direct interaction</td>
</tr>
<tr>
<td class="label">[Lithium](/therapeutics/lithium-tauopathy)</td>
<td>Both modulate GSK3β</td>
</tr>
<tr>
<td class="label">Diabetes medications</td>
<td>Curcumin may lower blood glucose</td>
</tr>
</table>
Evidence Rubric Score: 40/80
Pathway Diagram
Mermaid diagram (expand to render)
Overview
Curcumin (diferuloylmethane) is the principal polyphenolic curcuminoid from the rhizome of turmeric (Curcuma longa), constituting 2-8% of the dried root by weight. Along with the minor curcuminoids demethoxycurcumin (DMC) and bisdemethoxycurcumin (BDMC), it has been investigated extensively as a potential neuroprotective agent for [Alzheimer's disease](/diseases/alzheimers-disease) (AD), [Parkinson's disease](/diseases/parkinsons-disease) (PD), [progressive supranuclear palsy](/diseases/psp) (PSP), and other neurodegenerative conditions [@aggarwal2007].
The interest in curcumin for neurodegeneration stems from its multi-target pharmacology: direct inhibition of [amyloid-beta](/proteins/amyloid-beta) (Aβ) and [tau](/proteins/tau) aggregation, suppression of [NF-κB](/entities/nf-kb)-driven neuroinflammation, chelation of redox-active metal ions, and activation of [Nrf2](/genes/nrf2) cytoprotective pathways [@cole2007]. Epidemiological data from India and Southeast Asia — where dietary turmeric consumption is high — suggests substantially lower age-adjusted AD prevalence (4.4-fold lower in rural India compared to the United States), though confounding by diet, genetics, and lifestyle cannot be excluded [@ganguli2000].
However, curcumin presents a fundamental pharmacological challenge: its native oral bioavailability is less than 1% due to rapid intestinal glucuronidation, first-pass hepatic metabolism, and poor aqueous solubility [@anand2007]. This bioavailability crisis has necessitated the development of enhanced formulations (Longvida, Theracurmin, Meriva, BCM-95) that address absorption barriers, and has complicated interpretation of clinical trial results where different formulations, doses, and populations were studied. Curcumin is also classified as a pan-assay interference compound (PAINS) — a molecule that can produce false-positive results in many biochemical assays due to non-specific binding, aggregation, fluorescence, and chemical reactivity [@nelson2017]. This PAINS liability requires that mechanistic claims be interpreted with particular care.
Molecular Mechanisms
Anti-Amyloid Activity
Curcumin interacts with Aβ through multiple mechanisms [@yang2005]:
Direct fibril binding and disruption: Curcumin binds to the hydrophobic β-sheet structure of Aβ fibrils with a dissociation constant of approximately 1 μM. The diarylheptanoid scaffold spans two adjacent β-strands, disrupting intermolecular hydrogen bonding networks. In vitro, curcumin reduces Aβ42 fibril formation by 40-60% and can disaggregate pre-formed fibrils at micromolar concentrations [@yang2005].
Oligomer targeting: Curcumin preferentially binds toxic Aβ oligomers (the most neurotoxic species) over monomers or mature fibrils, potentially by stabilizing non-toxic off-pathway aggregates [@necula2007].
Amyloid PET imaging: Curcumin's Aβ-binding property has been exploited diagnostically — fluorescent curcumin derivatives (e.g., CRANAD-2) have been developed as amyloid PET tracers, confirming that the curcumin scaffold genuinely interacts with amyloid deposits in vivo [@ran2009].
Enhanced phagocytic clearance: Curcumin promotes [microglial](/cell-types/microglia) phagocytosis of Aβ by inducing CD36 and TREM2 expression while suppressing the pro-inflammatory (M1-type) microglial response — effectively redirecting microglia from neurotoxic inflammation to beneficial amyloid clearance [@zhang2006].Anti-Tau Activity
The tau anti-aggregation activity of curcumin is particularly relevant for tauopathies [@rane2017]:
Direct tau binding: Curcumin binds to the microtubule-binding repeat domain of tau (R1-R4), the same region that mediates tau self-assembly. The binding involves the PHF6 hexapeptide motif (VQIVYK) and the PHF6* motif (VQIINK), which are the nucleation seeds for paired helical filament formation [@rane2017].
Inhibition of tau aggregation: At 10-50 μM concentrations, curcumin inhibits heparin-induced tau polymerization by 50-80% in vitro and reduces pre-formed tau filament density by 30-50%[@masuda2011].
[GSK3β](/entities/gsk3-beta) modulation: Curcumin inhibits GSK3β activity (IC50 ~10 μM) both directly and through Akt activation, reducing tau phosphorylation at key disease-associated epitopes (Ser396, Ser404, Thr231, AT8)[@huang2014].
[4R-tau](/proteins/4r-tau) specificity: PSP and CBS are [4-repeat tauopathies](/entities/4r-tau). The PHF6 motif (VQIVYK) in the fourth microtubule-binding repeat is more aggregation-prone than the corresponding 3R-tau sequence, and curcumin's binding to this region may preferentially inhibit 4R-tau aggregation — a hypothesis that requires further experimental validation [@rane2017].NF-κB Suppression and Anti-Inflammatory Effects
Curcumin is one of the most potent natural inhibitors of the NF-κB signaling pathway [@jobin1999]:
- IKKβ inhibition: Curcumin directly inhibits IκB kinase β (IKKβ), preventing phosphorylation and degradation of IκBα, thereby keeping [NF-κB](/entities/nf-kb) sequestered in the cytoplasm
- p65 nuclear translocation block: Even when NF-κB is released, curcumin reduces p65 nuclear import by interfering with importin α/β recognition
- Downstream gene suppression: Results in decreased expression of TNF-α, [IL-6](/entities/il-6), IL-1β, [COX-2](/entities/cox2), iNOS, MCP-1, and MMP-9 — the key mediators of neuroinflammation
- Microglial polarization: Shifts [microglia](/cell-types/microglia) from pro-inflammatory (M1) to anti-inflammatory (M2) phenotype, promoting phagocytic Aβ clearance rather than neurotoxic cytokine release [@zhang2006]
Curcumin chelates redox-active metal ions through its β-diketone moiety and phenolic hydroxyl groups [@baum2004]:
- Cu²⁺ chelation: Prevents copper-catalyzed Aβ aggregation and ROS generation via Fenton-like chemistry (Cu¹⁺ + H₂O₂ → Cu²⁺ + OH· + OH⁻)
- Fe²⁺/Fe³⁺ chelation: Reduces iron-mediated oxidative stress and lipid peroxidation; may lower ferroptotic cell death in neurons
- Zn²⁺ modulation: Zinc promotes Aβ aggregation at physiological concentrations; curcumin's zinc chelation reduces Aβ precipitation in synaptic clefts
- This metal chelation is relevant for PSP, where brain iron accumulation in the [substantia nigra](/brain-regions/substantia-nigra) and [globus pallidus](/brain-regions/globus-pallidus) is elevated, contributing to oxidative damage [@baum2004]
Nrf2 Activation and Antioxidant Effects
Curcumin activates the [Nrf2-Keap1-ARE pathway](/mechanisms/nrf2-keap1-pathway) through electrophilic modification of Keap1 cysteine residues (similar to [sulforaphane](/therapeutics/sulforaphane-nrf2-neuroprotection) but with lower potency)[@balogun2003]:
- Induces HO-1, NQO1, GCL, and glutathione S-transferases
- Increases brain GSH levels by 15-25% in preclinical models
- Curcumin's direct radical scavenging (via phenolic OH groups) complements the enzyme-based antioxidant defense activated through Nrf2
Enhancement of DHA Synthesis
A distinctive mechanism: curcumin upregulates the expression of Δ-6-desaturase (FADS2) and elongase-2 enzymes in the liver, enhancing endogenous conversion of alpha-linolenic acid (ALA) to DHA by 50-70%[@wu2014]. This synergistic interaction with [omega-3 fatty acid](/therapeutics/omega-3-fatty-acids-neurodegeneration) metabolism may partly explain epidemiological benefits of curcumin-rich diets in populations with low fish consumption.
The Bioavailability Crisis
The Core Problem
Native curcumin has extremely poor oral bioavailability, estimated at <1% in humans [@anand2007]:
Aqueous insolubility: Curcumin is hydrophobic (LogP ~3.0); poorly absorbed from the aqueous environment of the intestinal lumen
Rapid glucuronidation: Intestinal UDP-glucuronosyltransferases (UGT1A1, UGT1A8) rapidly conjugate curcumin to curcumin glucuronide, a metabolite with uncertain bioactivity
First-pass hepatic metabolism: CYP450 reduction and phase II conjugation eliminate most absorbed curcumin before systemic circulation
Rapid plasma clearance: Even when plasma levels are achieved, half-life is only 30-45 minutesThis means that a typical 500 mg dose of native curcumin produces peak plasma concentrations of only 10-50 nM — 100-1000x below the concentrations required for Aβ/tau inhibition in vitro (1-50 μM)[@anand2007].
The industry response has been a proliferation of enhanced-bioavailability formulations, each using a different technology [@dei2019]:
Critical distinction: High plasma curcumin does not necessarily mean high brain curcumin. Longvida SLCP is the only formulation with published evidence of free (unconjugated) curcumin delivery to brain tissue in animal models [@gota2010]. Most other formulations achieve high plasma levels of curcumin glucuronides and sulfates, whose bioactivity in the CNS is uncertain.
Clinical Evidence
Alzheimer's Disease Trials
Theracurmin Memory Trial (Small et al., 2018)
The most cited positive trial: 40 non-demented adults aged 50-90 with mild memory complaints were randomized to Theracurmin (90 mg curcumin twice daily) or placebo for 18 months in a double-blind, placebo-controlled trial at UCLA [@small2017]. Results:
- Significant improvement in verbal memory (SRT, p=0.002) and visual memory (BVMT, p=0.01)
- Significant improvement in attention (Trail Making Test, p=0.01)
- FDDNP-PET imaging showed decreased tau and amyloid signal in amygdala and hypothalamus in the curcumin group
- Limitations: Very small sample size (N=40), memory complaints only (not MCI or AD), FDDNP-PET is not well-validated for tau imaging
ADCS Curcumin Trial (Ringman et al., 2012)
The largest dedicated AD trial: 36 patients with mild-to-moderate AD randomized to Curcumin C3 Complex (2g or 4g/day) or placebo for 24 weeks [@ringman2012]. Results:
- No significant differences on ADAS-cog, NPI, ADCS-ADL, MMSE
- Curcumin levels were detectable but low (plasma 7.32 ng/mL at 4g dose)
- High dropout rate (30%) due to GI side effects at high doses
- Conclusion: Native C3 Complex formulation likely inadequate for brain exposure; not a valid test of the curcumin hypothesis
Longvida Healthy Elderly Trial (Cox et al., 2015)
60 healthy adults aged 60-85 randomized to Longvida SLCP (400 mg/day, delivering 80 mg curcumin) or placebo for 4 weeks [@cox2015]. Results:
- Significant improvement in sustained attention and working memory at 1 hour post-dose (acute effects)
- Non-significant trends for chronic (4-week) cognitive improvement
- Reduced fatigue and improved calmness ratings
- Supports brain bioavailability of Longvida formulation but underpowered for chronic cognitive endpoints
Depression Trials (Indirect Evidence)
Several RCTs demonstrate curcumin's CNS bioactivity through depression outcomes:
- BCM-95 (1000 mg/day) produced antidepressant effects equivalent to fluoxetine (20 mg/day) in an 8-week RCT (N=60)[@sanmukhani2014]
- Meta-analysis of 10 RCTs (N=531) confirmed significant antidepressant effect (SMD −0.34, 95% CI −0.56 to −0.13), particularly in longer trials (≥6 weeks)[@fusarpoli2020]
- These results confirm that enhanced-bioavailability curcumin formulations achieve CNS-active concentrations, supporting their potential for neurodegeneration
Parkinson's Disease Evidence
No dedicated curcumin RCT for PD has been completed. Preclinical evidence is strong:
- Curcumin protects dopaminergic neurons in MPTP (40-60% protection), 6-OHDA, and rotenone PD models [@mythri2012]
- Reduces [alpha-synuclein](/proteins/alpha-synuclein) aggregation by binding to the non-amyloid component (NAC) domain and preventing β-sheet formation [@conway1998]
- Enhances DJ-1 expression and mitochondrial complex I activity in SH-SY5Y cells
- Reduces L-DOPA-induced dyskinesias in 6-OHDA-lesioned rats through modulation of striatal ΔFosB expression [@mythri2012]
CBS/PSP Relevance and Rationale
Tauopathy-Specific Considerations
The rationale for curcumin in PSP and CBS is based on its direct anti-tau mechanisms:
4R-tau aggregate disruption: PSP and CBS feature straight filaments and astrocytic/oligodendroglial [4R-tau](/proteins/4r-tau) inclusions. Curcumin's binding to the PHF6 motif in the fourth microtubule-binding repeat could inhibit the nucleation of these disease-specific tau strains. However, the required concentrations (10-50 μM) significantly exceed achievable brain levels (estimated 0.1-1 μM with Longvida), suggesting that only partial inhibition is plausible [@rane2017].
GSK3β-tau phosphorylation axis: Curcumin's inhibition of GSK3β — the primary kinase driving pathological tau phosphorylation at PSP-relevant epitopes — complements the mechanisms of [lithium](/therapeutics/lithium-tauopathy) and [omega-3 fatty acids](/therapeutics/omega-3-fatty-acids-neurodegeneration)[@huang2014].
Neuroinflammatory tufted astrocyte environment: PSP features prominent tufted [astrocyte](/cell-types/astrocytes) tau pathology with surrounding neuroinflammation. Curcumin's potent NF-κB suppression in astrocytes and microglia could reduce the inflammatory milieu that promotes tau propagation [@jobin1999].
Iron chelation in basal ganglia: PSP shows elevated iron in the [substantia nigra](/brain-regions/substantia-nigra), [subthalamic nucleus](/cell-types/subthalamic-nucleus), and [globus pallidus](/brain-regions/globus-pallidus). Curcumin's metal chelation properties could reduce iron-mediated oxidative damage and ferroptosis, complementing [deferiprone](/therapeutics/deferiprone-neurodegeneration) at lower potency but superior tolerability [@baum2004].
DHA synthesis enhancement: Curcumin's upregulation of hepatic FADS2 increases DHA availability, indirectly supporting omega-3-mediated neuroprotection — a synergistic combination for patients taking both supplements [@wu2014].CBS/PSP Implementation Considerations
Dosing Protocol
Based on formulation pharmacokinetics and available clinical evidence [@dei2019][@small2017][@cox2015]:
Critical notes:
- Always specify the formulation — "curcumin 500 mg" is meaningless without knowing the delivery technology
- Take with fat-containing meals to maximize absorption (even enhanced formulations benefit from dietary fat)
- Do NOT use piperine (BioPerine) formulations in patients on medications metabolized by CYP3A4, CYP2D6, or CYP1A2, as piperine inhibits these enzymes and can increase drug exposure [@bhardwaj2002]
Safety and Tolerability
Adverse Effects
Curcumin has an excellent safety profile with centuries of dietary use as turmeric [@lao2006]:
- Gastrointestinal: Most common (5-15%): nausea, diarrhea, abdominal discomfort. More frequent at doses >4g/day of native curcumin; less common with enhanced formulations at lower doses
- Hepatic: Rare reports of elevated liver enzymes with turmeric supplements (primarily contaminated products); a 2022 Italian case series raised concerns but implicated adulterated products, not pure curcumin [@lombardi2021]. FDA GRAS status maintained.
- Oxalate content: Turmeric powder (not curcumin extracts) contains calcium oxalate, which could contribute to kidney stones at very high turmeric doses. Curcuminoid extracts have negligible oxalate.
- Iron chelation: Theoretical concern for iron-deficient patients at high doses; curcumin's iron-binding affinity is much weaker than [deferiprone](/therapeutics/deferiprone-neurodegeneration). No clinical iron depletion reported.
- Anticoagulant effect: Curcumin has mild antiplatelet activity at high doses (>2g/day); exercise caution with concurrent anticoagulants.
Contraindications
- Active gallbladder disease (curcumin stimulates bile secretion)
- Iron deficiency anemia (theoretical; monitor ferritin if using >1g/day long-term)
- Scheduled surgery within 7 days (mild antiplatelet effect)
- Concurrent use of piperine-containing formulations with narrow therapeutic index drugs
Drug Interactions
The PAINS Concern
Curcumin is a prototypical PAINS (Pan-Assay Interference Compound) — a molecule that produces false-positive results in many biochemical screening assays [@nelson2017]. This is important context for interpreting its mechanistic literature:
Legitimate concerns:
- Curcumin aggregates in aqueous solution, forming colloidal particles that non-specifically inhibit enzymes
- It fluoresces, interfering with fluorescence-based assays
- It is chemically reactive (Michael acceptor), covalently modifying proteins non-specifically
- Many "curcumin targets" identified in high-throughput screens may be artifacts
Counterarguments supporting genuine activity:
- Aβ and tau binding confirmed by crystallography, solid-state NMR, and fluorescence anisotropy under non-aggregating conditions [@yang2005]
- In vivo effects in transgenic animals cannot be explained by in vitro assay artifacts
- PET imaging confirms amyloid-binding in human brain (FDDNP-PET studies)[@small2017]
- Anti-inflammatory effects confirmed by specific NF-κB pathway analysis, not generic protein inhibition
- Epidemiological associations cannot be attributed to PAINS activity
The balanced interpretation: curcumin has genuine biological activity, but the number of "targets" is likely overestimated by PAINS-confounded assay data. Its primary mechanisms are probably limited to Aβ/tau binding, NF-κB suppression, metal chelation, Nrf2 activation, and DHA synthesis enhancement [@nelson2017].
Combination Therapy Potential
Curcumin + [omega-3 DHA/EPA](/therapeutics/omega-3-fatty-acids-neurodegeneration): Curcumin enhances hepatic DHA synthesis (FADS2 upregulation) while omega-3s provide SPM-mediated inflammation resolution. This is the strongest evidence-based combination for curcumin [@wu2014].
Curcumin + [sulforaphane](/therapeutics/sulforaphane-nrf2-neuroprotection): Both activate Nrf2 through different mechanisms (curcumin via electrophilic Keap1 modification; sulforaphane via covalent Cys151 adduction). Combined, they may achieve Nrf2 activation at lower individual doses [@balogun2003].
Curcumin + [melatonin](/therapeutics/melatonin-tauopathy): Convergent anti-inflammatory and antioxidant mechanisms through distinct pathways; melatonin protects curcumin from oxidative degradation [@shimmyo2008].
Curcumin + [lithium](/therapeutics/lithium-tauopathy): Both target GSK3β — lithium via direct competitive inhibition (Ki ~2 mM) and curcumin via indirect Akt-mediated inhibition. Combined GSK3β suppression may enhance anti-tau efficacy [@huang2014].
Curcumin + exercise: Exercise increases BDNF, and curcumin enhances exercise-induced BDNF upregulation in animal models, potentially amplifying synaptic plasticity benefits [@vaynman2004].Implementation Workflow
Starting Curcumin for Neuroprotection
Formulation selection: Choose Longvida SLCP (preferred for CNS targeting) or Theracurmin (highest plasma levels). Avoid generic "curcumin 95%" without enhanced delivery.
Medication review: Check for CYP interactions if using piperine formulations; assess anticoagulation status
Initiation: Start at 400 mg Longvida (1 capsule) once daily with a fat-containing meal for 1 week
Dose escalation: Increase to 400 mg twice daily if tolerated; maximum 800 mg twice daily
Monitoring: No routine blood monitoring needed; check LFTs if symptoms suggest hepatic effects; assess cognitive status at 3-6 months
Combination: Add omega-3 DHA/EPA for synergistic DHA enhancement; consider [sulforaphane](/therapeutics/sulforaphane-nrf2-neuroprotection) for enhanced Nrf2 activationDecision Framework for CBS/PSP Patients
Early diagnosis, motivated patient? → Longvida 400mg BID + omega-3 2g/day + CoQ10
Moderate disease, on multiple meds? → Longvida 400mg daily; avoid piperine formulations
Dysphagia developing? → Open Longvida capsule into applesauce/yogurt; or Theracurmin liquid
Already on lithium? → Continue both; monitor GSK3β-related effects (no specific test available)
Iron-deficient? → Use lower curcumin dose (400mg/day); monitor ferritin
Budget-limited? → BCM-95 1000mg/day is more affordable; less CNS evidence
See Also
- [Nrf2 Activators for Neurodegenerative Diseases](/therapeutics/nrf2-activators-neurodegeneration)
- [NRF2-KEAP1 Oxidative Stress Response Pathway](/mechanisms/nrf2-keap1-pathway)
- [Omega-3 Fatty Acids for Neurodegeneration](/therapeutics/omega-3-fatty-acids-neurodegeneration)
- [Sulforaphane and Nrf2 Activation](/therapeutics/sulforaphane-nrf2-neuroprotection)
- [Lithium for Tauopathy](/therapeutics/lithium-tauopathy)
- [Deferiprone for Neurodegeneration](/therapeutics/deferiprone-neurodegeneration)
- [Melatonin for Tauopathy](/therapeutics/melatonin-tauopathy)
- [CBS/PSP Treatment Rankings](/therapeutics/cbs-psp-treatment-rankings)
- [Amyloid-Beta](/proteins/amyloid-beta)
- [Tau Protein](/proteins/tau)
- [Microglia](/cell-types/microglia)
- [GSK3-Beta](/entities/gsk3-beta)
External Links
- [Wikipedia](https://en.wikipedia.org/)
- [NCBI Resources](https://www.ncbi.nlm.nih.gov/)
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[Sanmukhani J, Satodia V, Trivedi J, et al, Efficacy and safety of curcumin in major depressive disorder: a randomized controlled trial (2014)](https://doi.org/10.1002/ptr.5025)
[Fusar-Poli L, Vozza L, Gabbiadini A, et al, Curcumin for depression: a meta-analysis (2020)](https://doi.org/10.1080/10408398.2020.1753885)
[Mythri RB, Bharath MM, Curcumin: a potential neuroprotective agent in Parkinson's disease (2012)](https://doi.org/10.2174/187152712802762489)
[Conway KA, Harper JD, Lansbury PT, Accelerated in vitro fibril formation by a mutant α-synuclein linked to early-onset Parkinson disease (1998)](https://pubmed.ncbi.nlm.nih.gov/9843958/)
[Bhardwaj RK, Glaeser H, Becquemont L, Klotz U, Gupta SK, Fromm MF, Piperine, a major constituent of black pepper, inhibits human P-glycoprotein and CYP3A4 (2002)](https://doi.org/10.1124/jpet.102.039495)
[Lao CD, Ruffin MT, Normolle D, et al, Dose escalation of a curcuminoid formulation (2006)](https://doi.org/10.1186/1472-6882-6-10)
[Lombardi N, Crescioli G, Maggini V, et al, Acute liver injury following turmeric use in Tuscany: an analysis of the Italian Phytovigilance database and systematic review of case reports (2021)](https://doi.org/10.1017/S000711452000345X)
[Shimmyo Y, Kihara T, Akaike A, Niidome T, Sugimoto H, Multifunction of myricetin on A beta: neuroprotection via a conformational change of A beta and reduction of A beta via the interference of secretases (2008)](https://doi.org/10.1016/j.neulet.2008.02.009)
[Vaynman S, Ying Z, Gomez-Pinilla F, Hippocampal BDNF mediates the efficacy of exercise on synaptic plasticity and cognition (2004)](https://doi.org/10.1111/j.1460-9568.2004.03720.x)From the [SciDEX Exchange](/exchange) — scored by multi-agent debate
- [Nutrient-Sensing Epigenetic Circuit Reactivation](/hypothesis/h-4bb7fd8c) — <span style="color:#81c784;font-weight:600">0.79</span> · Target: SIRT1
- [CYP46A1 Overexpression Gene Therapy](/hypothesis/h-2600483e) — <span style="color:#81c784;font-weight:600">0.79</span> · Target: CYP46A1
- [Circadian Glymphatic Entrainment via Targeted Orexin Receptor Modulation](/hypothesis/h-9e9fee95) — <span style="color:#81c784;font-weight:600">0.77</span> · Target: HCRTR1/HCRTR2
- [Selective Acid Sphingomyelinase Modulation Therapy](/hypothesis/h-de0d4364) — <span style="color:#81c784;font-weight:600">0.77</span> · Target: SMPD1
- [Membrane Cholesterol Gradient Modulators](/hypothesis/h-9d29bfe5) — <span style="color:#81c784;font-weight:600">0.76</span> · Target: ABCA1/LDLR/SREBF2
- [Microbial Inflammasome Priming Prevention](/hypothesis/h-e7e1f943) — <span style="color:#81c784;font-weight:600">0.76</span> · Target: NLRP3, CASP1, IL1B, PYCARD
- [Blood-Brain Barrier SPM Shuttle System](/hypothesis/h-959a4677) — <span style="color:#81c784;font-weight:600">0.75</span> · Target: TFRC
- [Purinergic Signaling Polarization Control](/hypothesis/h-0758b337) — <span style="color:#81c784;font-weight:600">0.74</span> · Target: P2RY1 and P2RX7
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