halfmarble | SteadyDoseTool

SteadyDoseTool — Pharmacokinetic Simulation

Bateman model: C(t) = A(e^-ke·t - e^-ka·t) — click chart to set NOW, then add doses

FOR EDUCATIONAL AND RESEARCH PURPOSES ONLY. This simulation is not medical advice. It does not account for individual physiology, drug interactions, or clinical context. Always consult your physician before making any changes to your medication schedule.

2:00 PM NOW — drag on chart to move

Activity Demand — click/drag to paint

DYSKINESIA TOLERANCE

Eating Windows — doses during meals use reduced absorption

Meal 1 3:00 PM – 4:00 PM

Meal 2 12:00 PM – 1:00 PM

Meal 3 8:00 AM – 9:00 AM

DOSES TODAY 0

CURRENT LEVEL 0%

TIME IN RANGE —

NEXT DOSE IN —

VARIABILITY ±50%

Confidence band (population variability in absorption & elimination)

Therapeutic window (effective range without dyskinesia)

Expected blood concentration (Bateman equation)

Fasting dose — auto-detected from eating windows, faster absorption

Circadian zones — morning peak (best absorption), afternoon dip (wearing off risk), wind-down

Activity demand — modulates therapeutic window (higher demand = higher coverage needed)

Eating window — reduced levodopa absorption (protein competes for LNAA transport)

Glass Box // what the AI reads

No black box. Every paper and data source behind the pharmacokinetic model is listed here. You see what the math sees — nothing hidden, nothing invented. The source code will be released for independent review.

ANCHORED The PK model is pinned to published pharmacokinetic parameters — not a drifting LLM. The math cannot silently change between updates.

ON-DEVICE The PK model runs on your phone. No cloud. No server. All computation is local.

LOCAL Your dose logs and subjective reports stay on your phone by default. Join the fight beyond your own case: opt in to share anonymized, aggregated patterns with researchers — never your identity, never automatic, never without consent. See exactly what gets shared →

TRACEABLE Every parameter in the Bateman equation traces to a published source below. If it's not in the Glass Box, the model won't use it.

Pharmacokinetic Model Sources

01 Pharmacokinetics of levodopa Nutt & Fellman — Movement Disorders, 1993

02 IPX066 (Rytary): pharmacokinetics of extended-release carbidopa-levodopa Hauser et al. — Neurology, 2013

03 Continuous dopaminergic stimulation in Parkinson's disease Olanow et al. — The Lancet Neurology, 2006

04 Population pharmacokinetics of levodopa in Parkinson's disease patients Clinical Pharmacokinetics, 2020

05 Sinemet CR pharmacokinetics: bioavailability and absorption characteristics Movement Disorders, 2014

06 Effect of food on the pharmacokinetics of levodopa formulations Parkinsonism & Related Disorders, 2016

Clinical Framework

07 Low-fat versus ketogenic diet in Parkinson's disease: A pilot randomized controlled trial Phillips et al. — Movement Disorders, 2018

08 Wearing off and motor complications in Parkinson's disease Stocchi et al. — Neurology, 2010

09 Motor fluctuations and dyskinesia in Parkinson's disease: clinical guide and practical tips Vijayakumar & Jankovic — The Lancet Neurology, 2018

10 Bateman, H. — The solution of a system of differential equations in pharmacokinetics Proc. Cambridge Phil. Soc., 1910

Simulation Parameters Derived From

Sinemet IR: t½ 90 min, Tmax 30-60 min, F=99% — from FDA prescribing label + Nutt & Fellman (1993)
Sinemet CR: t½ 90 min, Tmax 120 min, F=71% — from FDA prescribing label + controlled-release PK studies
Rytary ER: dual-phase absorption (60% fast / 40% slow), Tmax 1h/4h — from Hauser et al. (2013) + FDA label
Food effect: high-protein meals delay Tmax by ~30 min, reduce Cmax — from competitive amino acid transport literature

GLASS_BOX_POLICY: Every parameter in this simulation traces to a published pharmacokinetic source. The Bateman equation is the standard one-compartment oral absorption model used in clinical pharmacology. No proprietary algorithms. No hidden tuning. No synthetic data.