Curcumin (with Piperine/Liposomal) vs Pregnenolone

Mechanism

Curcumin modulates over 100 molecular targets. Primary mechanisms include direct inhibition of NF-kB nuclear translocation (master inflammatory transcription factor), suppression of COX-2 and iNOS expression, inhibition of STAT3 and AP-1 signaling, and activation of Nrf2-ARE pathway upregulating Phase II detoxification enzymes (glutathione S-transferase, heme oxygenase-1). It also inhibits mTOR signaling and modulates epigenetic enzymes (HATs, HDACs, DNMTs).

Standard Dosing

500-1000mg curcuminoids daily (enhanced bioavailability form)

Timing

With meals containing fat. Piperine enhances absorption 2000% but also affects drug metabolism.

Cycle Duration

ongoing

Side Effects

• GI upset/diarrhea at high doses
• Yellow staining of teeth/skin
• Rare: contact dermatitis
• Potential iron depletion with chronic high-dose use

Contraindications

• Gallbladder obstruction/gallstones (stimulates bile flow)
• Iron-deficiency anemia (chelates iron)
• Scheduled surgery (discontinue 2 weeks prior)
• Pregnancy at therapeutic doses

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Mechanism

Pregnenolone is the 'master steroid' synthesized from cholesterol via CYP11A1 (side-chain cleavage enzyme) in adrenal glands, gonads, and brain. It serves as the biosynthetic precursor to all steroid hormones (progesterone, DHEA, cortisol, testosterone, estradiol, aldosterone). In the CNS, pregnenolone and its sulfated derivative (pregnenolone sulfate) function as potent neurosteroids: pregnenolone sulfate is a positive allosteric modulator of NMDA receptors enhancing glutamatergic neurotransmission, a negative modulator of GABA-A receptors (increasing neural excitability), and an activator of TRPM3 calcium channels. It also modulates sigma-1 receptors involved in neuroplasticity.

Standard Dosing

Research indicates 10-50 mg daily orally for neurosteroid and cognitive support. Clinical trials in schizophrenia used up to 500 mg/day.

Timing

Morning dosing preferred (aligns with diurnal cortisol rhythm). Sublingual may provide faster onset and better bioavailability. Take with or without food.

Cycle Duration

Ongoing with periodic reassessment. Cycle 5 days on / 2 days off, or 3-4 weeks on / 1 week off to prevent downstream hormone accumulation.

Side Effects

• Headache
• Irritability/mood changes
• Insomnia
• Acne (via androgenic metabolites)
• Heart palpitations
• Hair loss (if converting heavily down androgen pathway)
• Overstimulation
• Overstimulation and anxiety (from GABA-A antagonism at higher doses)
• Insomnia (if taken late in the day)
• Acne (from downstream androgen conversion)
• Irritability
• Hair growth or loss (from downstream hormonal changes)

Contraindications

• Hormone-sensitive cancers
• Seizure disorders (complex GABA modulation)
• Pregnancy
• PCOS
• Concurrent HRT without monitoring
• Use only with lab-guided supervision
• Hormone-sensitive cancers (breast, prostate, ovarian — due to downstream conversion)
• History of seizures (pregnenolone sulfate is pro-excitatory)
• Pregnancy and breastfeeding
• Bipolar disorder (may exacerbate manic episodes)

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