Substance and claimed effects

Post-meal sleepiness — clinical term postprandial somnolence, lay terms food coma, the afternoon dip, the post-lunch dip — is the drop in alertness, motivation, and cognitive throughput that follows eating, especially in the 30–180 minutes after a larger meal. The phenomenon is near-universal across healthy adults Monk 2005, with subjective and objective measures of daytime sleepiness rising sharply after lunch and a measurable share of the effect persisting beyond what a simple "circadian dip" predicts Wells & Read 1996. The entry covers the substance (eating a meal) and the meaningful consequences that follow from it: a felt drop in energy and focus for one to three hours, downstream effects on driving and work safety, and the leverage available from modulating meal size, composition, timing, and the immediate post-meal hour. Out of scope: clinical hypersomnia, narcolepsy, and reactive hypoglycemia as primary conditions (each warrants its own entry; flagged in editor notes).

Evidence by addressing question

mechanism

Four mechanisms contribute, in rough order of evidentiary weight. None is the whole story; the dip is a confluence.

Circadian timing. The suprachiasmatic nucleus drives a biphasic alertness curve with a trough in the early afternoon — roughly 1pm to 3pm — independent of whether a meal was eaten Monk 2005, Cajochen et al. 1999. Forced-desynchrony studies in which meals are decoupled from clock time still show the afternoon trough, locating part of the effect in central circadian rhythm rather than digestion. This is the floor: even with no lunch, alertness drops in the early afternoon.

Orexin / hypocretin suppression by rising glucose. Lateral-hypothalamic orexin neurons — the master switch for wakefulness — are directly inhibited by glucose via tandem-pore potassium channels Burdakov et al. 2006. In mice, orexin neuron firing tracks energy state: low glucose and low leptin activate them; rising glucose and rising leptin silence them Yamanaka et al. 2003. Orexin loss in humans is narcolepsy Stahl 2010. A meal that lifts plasma glucose pushes the same lever, just transiently and less profoundly. This is the cleanest single mechanism linking food intake to sleepiness, and it explains why a high-glycemic meal that produces a large glucose excursion provokes a stronger dip than the same calories delivered as protein or fat.

Parasympathetic / vagal dominance after eating. A meal triggers a shift toward parasympathetic activity to support digestion: gastric distension, splanchnic blood-flow rise, and cholecystokinin release all increase vagal tone Bazar et al. 2004. Subjective sleepiness correlates with the magnitude of this autonomic shift across meal types. In susceptible populations — the elderly, autonomic dysfunction — this can drop blood pressure measurably (postprandial hypotension) and produce frank somnolence rather than a mild dip Jansen & Lipsitz 1995.

Tryptophan / serotonin pathway. A high-carbohydrate, low-protein meal raises the plasma ratio of tryptophan to other large neutral amino acids — insulin clears the competitors from blood faster than it clears tryptophan — increasing tryptophan transport across the blood-brain barrier and serotonin synthesis in the brain Spring et al. 1987, Wurtman & Wurtman 1995. Acute oral tryptophan dosing reliably increases subjective sleepiness Hartmann 1982. The mechanism is real but quantitatively smaller than the orexin and circadian pathways for ordinary meals; it matters more for very-high-carb, low-protein lunches than for mixed plates.

evidence

The phenomenon itself replicates whenever it is measured. Wells & Read fed healthy adults a 1,000-kcal lunch and a 300-kcal lunch on different days; both objective (Multiple Sleep Latency Test) and subjective sleepiness were greater after the larger meal, with the effect peaking around 60–120 minutes post-meal Wells & Read 1996. Reyner et al. extended the design into a monotonous driving simulator and found that a larger lunch produced measurably more lane drift, more sleep-related driving incidents, and more EEG-defined drowsiness than a smaller one — a real-world endpoint, not just a vigilance task Reyner et al. 2012. Orr et al. tested high-fat vs balanced lunches and found higher sleepiness after the high-fat meal at equivalent calories, implicating composition independent of size Orr et al. 1997. Cunliffe et al. compared mixed, pure-carbohydrate, and pure-fat meals and found all three produced fatigue, with the mixed and pure-carb meals more sleep-promoting than pure fat Cunliffe et al. 1997. Afaghi et al. showed that a high-glycemic-index carbohydrate meal four hours before bed shortened sleep onset compared to a low-GI version — same mechanism, different time-of-day endpoint Afaghi et al. 2007. Monk's review of the post-lunch dip integrates the evidence and concludes that meal size and composition modulate, but do not cause, the basal circadian dip Monk 2005. The mechanism layer is animal and human-tissue work on orexin Burdakov et al. 2006, Yamanaka et al. 2003.

protocol

Three levers move the dip, with effect sizes large enough to be felt and small enough not to abolish the underlying circadian trough. Meal size: trim midday calories — the Wells & Read 700-kcal difference between large and small lunch is roughly the difference between a full restaurant lunch and a normal plate Wells & Read 1996, Reyner et al. 2012. Composition: shift the macros toward protein and unrefined carbohydrate; minimize refined-starch + added-sugar loads that drive the largest glucose excursions and the largest orexin suppression Afaghi et al. 2007, Holt et al. 1995. Post-meal walking: 10–15 minutes of light walking after a meal blunts the glucose excursion measurably DiPietro et al. 2013; the mechanism (muscle GLUT4 translocation) directly addresses the orexin-suppression pathway. If the dip lands anyway: a brief nap of 10–20 minutes (no longer, to avoid slow-wave sleep) substantially restores alertness without the deep-nap hangover; longer naps cause sleep inertia that costs more than they recover Brooks & Lack 2006. Caffeine works too, with the constraint that anything past about noon for a 2pm dip cuts into nighttime sleep — the half-life is ~5 hours, so a 2pm coffee still has a quarter of its load active at midnight.

contraindications

For the typical reader, no contraindications to the mitigations themselves. The severity of post-meal sleepiness, however, can flag underlying conditions: postprandial hypotension in older adults and people with autonomic dysfunction (Parkinson's, diabetic autonomic neuropathy) — a drop of ≥20 mmHg systolic within two hours of a meal is the diagnostic threshold, and the symptom is disabling rather than mild Jansen & Lipsitz 1995. Reactive hypoglycemia, less common than feared, produces dip symptoms 2–4 hours post-meal (later than the standard dip), often with shakiness and adrenergic features. Narcolepsy and idiopathic hypersomnia sit at the clinical end — irresistible sleep attacks, including after small meals, that don't respond to brief naps the way ordinary postprandial sleepiness does Stahl 2010. The clinical referral threshold: when the dip is dangerous (driving, machinery), disproportionate to meal size, or accompanied by cataplexy, sleep paralysis, or fainting.

misconceptions

Several widely-repeated stories are partially or entirely wrong. "Turkey makes you sleepy because of tryptophan" — turkey's tryptophan content is unremarkable among meats and lower than several seeds and cheeses Wurtman & Wurtman 1995. The Thanksgiving dip is a 2,000+ kcal meal with substantial wine and a long-stable circadian rhythm hitting its mid-afternoon floor; turkey is a bystander. "Blood goes to your stomach so your brain gets less" — splanchnic blood flow does rise after a meal, but total cerebral perfusion is regulated tightly and does not drop appreciably in healthy adults. The blood-to-the-gut story is folk physiology; the real mediators are neural (orexin, parasympathetic) and humoral (insulin, CCK, the tryptophan ratio) Bazar et al. 2004. "Sleepy after lunch means you have diabetes" — the typical postprandial dip is normal physiology; a severe, disproportionate dip with shakiness is a reason to investigate glucose regulation, but mild sleepiness after a normal meal is not a screening trigger.

audience

Most adults experience this. The dip is consistently steeper in older adults — partly through postprandial hypotension prevalence, partly through reduced orexin tone with age Jansen & Lipsitz 1995, Stahl 2010. Shift workers and the sleep-deprived experience the dip more severely because circadian and homeostatic sleep pressure stack with the meal-induced suppression of orexin Cajochen et al. 1999, Buxton et al. 2012. People on high-refined-carbohydrate diets get larger excursions and steeper dips. Cultures with siesta traditions (Mediterranean, Latin American) have built the dip into the workday rather than fighting it; cultures with continuous-workday norms experience it as a productivity loss.

alternatives

Alternatives to direct mitigation: eat the larger meal at the end of the day, when the dip's productivity cost is zero. Schedule low-demand work for the dip window — email triage, routine meetings, physical tasks — and protect the morning/late-afternoon peaks for deep work; this matches what laboratory cognitive performance data predicts Monk 2005, Lieberman 2003. Caffeine timing works but trades against night sleep — a pre-dip 100–150 mg coffee around noon catches the dip with minimal night cost Brooks & Lack 2006. Each of these has its own entry candidate (timed eating, chronotype-aware scheduling, strategic caffeine).

failure-modes

The mitigations fail when a reader treats the dip as a willpower problem and stacks caffeine across the afternoon — by 4pm a 200 mg afternoon coffee leaves a 50 mg load active at 1am, fragmenting sleep, which raises tomorrow's dip via increased homeostatic pressure. Other common failures: napping past 25–30 minutes and entering slow-wave sleep, then waking groggy Brooks & Lack 2006; eating an even larger lunch the day after a poor night's sleep (drowsiness is partly an orexin-low signal, which biases food choice toward calorically dense options) Reichelt et al. 2015; switching to "no lunch" and then crashing at 5pm on a glucose floor.

practicalities

All mitigations are free or near-free. A timer for nap duration (phone alarm) and a willingness to walk for 10–15 minutes after lunch are the entire equipment list. The harder constraint is social: a smaller lunch on a workday with a fixed lunch hour can feel undersized; eating with colleagues makes composition choices public; a 15-minute walk requires the lunch window to allow it. None of these are physical barriers; they're scheduling and culture.

stakes

For the median reader, the dip costs roughly 1–3 hours per day of degraded cognitive output — five to fifteen hours a week, around 250–750 hours a year. Driving data is the dramatic version: post-lunch monotonous driving produced measurably more drowsy-driving incidents than the same drive without the meal Reyner et al. 2012, and post-lunch is a real safety window. Long-term, the habit of medicating the dip with sugar plus caffeine drives chronic sleep fragmentation, which compounds: poorer night sleep produces a worse next-day dip, which produces more medication. The downstream metabolic cost — repeated large refined-carbohydrate lunches as the recurring stimulus — is the silent track underneath the felt one Buxton et al. 2012.

payoff

The recovered afternoon is the visible payoff. Adults who reorganize lunch report sustained focus into the 3pm–5pm window — the time of day most desk workers experience as throwaway. Subjective: the version of the day where the second half is as productive as the first. Objective: glycemic excursions blunt across weeks (a real metabolic improvement, even if small per meal) DiPietro et al. 2013, and the caffeine load drops, which compounds into better nighttime sleep and a lower next-day dip — a positive feedback loop on alertness rather than the negative one most readers are stuck in.

out-of-scope

Adjacent topics that warrant their own entries: meal timing as it intersects with sleep (late-night eating, time-restricted eating); chronotype-aware work scheduling; postprandial hypotension as a clinical entity in older adults; idiopathic hypersomnia and narcolepsy; glycemic-index management as a metabolic intervention beyond the dip. Flagged in editor notes.

The credibility range

Optimist case. The phenomenon is real, replicated across multiple labs and designs, has a clean mechanistic story converging on orexin suppression by glucose, and yields to simple modifications with measurable effect sizes. The driving simulator data demonstrates a real-world endpoint, not just a vigilance score Reyner et al. 2012. The orexin / glucose link supplies the missing molecular bridge between meals and sleepiness that older mechanism debates lacked Burdakov et al. 2006. Mitigations — smaller lunch, mixed macros, post-meal walking, a brief nap — are free, low-effort, and have additive effects. This is one of the highest-yield, lowest-cost behavioral levers for daytime function in the catalogue, especially for desk workers.

Skeptic case. Most of the effect on the typical reader is the circadian dip; the meal modulates a curve that would have dipped anyway Monk 2005. The mitigation studies have small samples and rarely measure productivity directly. The orexin story is largely animal work; the inference to human afternoon sleepiness involves a long extrapolation Yamanaka et al. 2003. Effect sizes for behavioral mitigations are modest. Treating the dip as a problem to fix may itself be a cultural artifact — siesta cultures suggest the productive response is to schedule around it, not to engineer it away. And the medicalization risk: a normal physiological dip becomes a thing to optimize, drawing attention away from larger sleep-debt issues that drive the same symptom.

Author's call. Both are right partially. The dip is partly circadian (baseline, unmodifiable) and partly meal-induced (real, modifiable, dose-dependent on meal size and composition). The mitigations have honest, modest effect sizes — not transformative, but free, additive, and reliably positive for typical readers. The orexin story is mechanistically the cleanest single thread but the human evidence is mostly correlational; mechanism is what makes the rest of the picture coherent rather than what carries the protocol. The entry leans practical: name the phenomenon as normal physiology, name the mechanism in plain terms, give the reader the modulator dial. Score evidence at 3 — the phenomenon and the basic mitigation effects are well-replicated, but the body of work is not RCT-dense at the level of guideline-grade interventions, and the mechanism inference involves animal data.

Stakeholder + incentive map

• Cognitive-enhancement and "biohacker" subculture: incentive to frame the dip as an enemy to defeat and to sell products (specialty coffee, nootropics, fasting protocols). The behavioral mitigations crowd out the products.
• Continuous-glucose-monitor industry: commercial interest in framing every glucose excursion as a problem. The underlying physiology is real, but the marketing overshoots the evidence.
• Workplace culture: the continuous workday model (no siesta) treats the dip as a productivity problem rather than a circadian fact. The unspoken incentive is to extract afternoon output even when biology is against it.
• Mainstream sleep medicine: tends to focus on nighttime sleep and pathological hypersomnia; the ordinary post-meal dip is undertreated as a topic because it is not pathology.
• Siesta-culture traditions: the cultural opposite — building the dip into the day. Useful counterpoint to the optimization frame.

Population variability

• Age. Steeper, longer dips in older adults; postprandial hypotension is a clinically meaningful version in 60+ readers, especially with hypertension medications Jansen & Lipsitz 1995. Orexin tone declines with age Stahl 2010.
• Baseline sleep status. Sleep-restricted readers experience a much steeper dip — the circadian and homeostatic pressures stack Cajochen et al. 1999. The dip is partly a signal of cumulative sleep debt; fixing the night sleep is upstream of fixing the dip.
• Habitual diet. High-refined-carbohydrate diets produce larger excursions and steeper dips. Mixed Mediterranean-pattern eaters show smaller excursions.
• Shift work and circadian misalignment. The dip lands at a different clock time depending on phase; mitigations have to map to internal time, not external time Buxton et al. 2012.
• Sex and chronotype. Smaller and less-studied effects; chronotype shifts the timing of the trough by ~1–2 hours in extreme morning vs evening types.
• Clinical conditions. Narcolepsy (orexin deficient), idiopathic hypersomnia, untreated obstructive sleep apnea, untreated depression, and uncontrolled diabetes all produce more severe and less mitigation-responsive dips.

Knowledge gaps

The big gap is human evidence for the orexin / glucose mechanism in real-world meals — the molecular link is well-characterized in rodents and slice preparations, but direct in vivo human measurement of hypothalamic orexin activity around meals is not feasible with current tools. Effect sizes for behavioral mitigations on long-term productivity or metabolic outcomes are under-quantified — most studies measure acute sleepiness or single-meal glucose excursions, not multi-week productivity or HbA_1c change. The contribution of macronutrient composition independent of total caloric load is poorly disentangled; Orr 1997 and Cunliffe 1997 disagree in detail. There is no good study of "what's the optimal lunch for an office worker" framed as a randomized trial with productivity endpoints — the literature is fragmented across nutrition, sleep, and ergonomics specialties.

Scope decisions. The brief named drowsiness after eating and four named factors (meal size, composition, blood sugar, circadian timing, digestion). All four covered in the body: meal size and composition under protocol and evidence; glucose / orexin and parasympathetic / digestion mechanisms under mechanism; circadian timing as the unmodifiable floor in mechanism and audience. No silent narrowing.

Action choice. Lands on do rather than know. The phenomenon needs explaining (which earns the model), but the entry's leverage is behavioural — three dials a reader can move — so do is honest about what the article is asking of them. Cadence daily follows.

Tryptophan citation odd ref. The Hartmann 1982 paper on L-tryptophan and sleep is stored under Buchsbaum2009 in the citation library — the ref name doesn't match the author/year of the underlying work. Cited visibly as "Hartmann 1982" in the article; flagging here so a future librarian can either rename or leave alone.

Bes-Rastrollo ref mismatch. Same pattern: Bes-Rastrollo2008 stores the Bazar et al. 2004 parasympathetic-mechanism paper. Cited visibly as "Bazar et al. 2004". Same flag.

Rating difficulties. energy and focus both at 4 felt right — this entry's whole gravity is "an afternoon you'd otherwise write off" — but a case for 3 exists if you think the dip is mostly circadian and the meal contribution is small. The author's call (research §3c) lands practical: the meal contribution is real and dose-dependent enough to earn the 4. longevity at 1 because the long-term metabolic mechanism is plausible but small per meal; not honest to score higher on indirect compounding alone. evidence at 3 reflects strong phenomenon replication but a mechanism story still resting on animal data.

Overall ≈ 46 on the dream-tier formula (applicability 5, energy 4, focus 4, effort/cost low, evidence 3). Dream narrative obligatory; written with a relief / recovery lever (afternoons gotten back) rather than aspiration. The dek and tagline pull from it: the tagline compresses the three-dial protocol; the dek leads with the felt scene of the lost afternoon.

Separate-entry candidates.

• Postprandial hypotension as a clinical entity in older adults — own entry, action know or respond, audience-scoped 60+. Flagged in body's contraindications.
• Strategic short naps — the 10–20 minute protocol deserves its own entry; called out here only as a rescue option.
• Caffeine half-life and timing — the afternoon-coffee-into-night-sleep loop is one of the highest-leverage interventions and warrants standalone treatment.
• Time-restricted eating / meal timing — adjacent and frequently confused with this entry.
• Chronotype-aware work scheduling — the "schedule around the dip" alternative deserves its own development.
• Idiopathic hypersomnia and narcolepsy — clinical-end conditions only flagged here for the severity-as-signal use.

Future links. Wire to entries above once they exist; also to any general entries on glycemic control, sleep debt, and circadian alignment when present.

Anti-medicalization note. Deliberate restraint on the CGM / quantified-self framing — the postprandial-glucose-monitoring industry has commercial incentive to convert every excursion into a problem, and the article should not pile onto that. The phenomenon is normal physiology with modulable dials, not a defect to instrument.