Featured condition · MCAS

Mast Cell Activation Syndrome

A multi-system inflammatory condition commonly misattributed to anxiety or allergy — and central to the hypermobility-dysautonomia-MCAS triad we see in a substantial fraction of complex cases.

Overview

What we mean when we say MCAS.

MCAS is a disorder of inappropriate mast cell activation: immune cells releasing histamine, tryptase, leukotrienes, prostaglandins, and other mediators without an appropriate allergic trigger. The result is a multi-system symptom picture spanning cutaneous, gastrointestinal, cardiovascular, neurologic, and respiratory domains.

MCAS frequently co-occurs with POTS and hypermobile EDS — a triad often described in current literature as a syndromic hub rather than three separate conditions. Overlap with SIBO, gastroparesis, and autoimmune features is common, and the integrated picture changes treatment strategy materially.

The condition predominantly affects women, onset most often in the 30s–50s, with median diagnostic delays of many years. Patients are routinely routed to allergy, psychiatry, or GI — rarely to the smaller set of clinicians who recognize the syndrome as its own entity.

Why it’s hard to navigate

The pattern we see in MCAS cases.

01
No universal diagnostic consensus. Major frameworks — Afrin/Molderings consensus II, the Akin/Valent proposal, and regional variants — differ on criteria, biomarkers, and treatment thresholds. Which framework your clinician uses changes whether you have a diagnosis.
02
Laboratory markers (serum tryptase, urinary mediator metabolites) are often normal, and require specific timing, sample handling, and clinical context to be interpretable. A normal test does not rule out MCAS.
03
Treatment is step-wise and highly individual — H1 and H2 blockers, mast-cell stabilizers, leukotriene modulators, low-dose naltrexone, and trigger management each have a role in different cases.
04
Most allergists and immunologists outside academic centers are unfamiliar with MCAS as distinct from systemic mastocytosis. Patients are frequently told they're fine or dismissed to psychiatry before reaching an MCAS-aware clinician.

Signals we look for

The Ternary Signal Library for MCAS.

Our Signal Library codifies the specific patterns that matter in MCAS — labs, genetic variants, imaging findings, symptom clusters, and comorbidity combinations. Your case is mapped against these signals in Stage 4 of the workflow; each activated signal is weighted and prioritized for your presentation.

Symptom clusters

—Cutaneous — flushing, urticaria, pruritus, dermographism
—GI — diarrhea, reflux, abdominal pain, food intolerances
—Cardiovascular — tachycardia episodes, hypotension, syncope
—Neurologic — brain fog, headache, paresthesia
—Respiratory — nasal congestion, wheeze, dyspnea
—Episodic pattern — trigger, severity, duration mapping

Laboratory markers

—Serum tryptase — baseline and timed post-episode
—Urinary N-methylhistamine, prostaglandin D2 metabolites
—Urinary leukotriene E4
—CBC with differential (eosinophils, basophils)
—Total IgE and specific IgE panels
—Chromogranin A

Trigger & environment audit

—Food triggers — high-histamine, high-tyramine, salicylate
—Chemical / fragrance / environmental triggers
—Temperature, exercise, stress triggers
—Medication sensitivities
—Hormonal cycle correlations

Triad & comorbidities

—POTS — autonomic testing, tilt table findings
—hEDS — Beighton, 2017 criteria
—GI dysmotility — gastroparesis, SIBO
—Small fiber neuropathy
—Autoimmune features — ANA, thyroid antibodies

How we approach it

The Ternary Health approach to MCAS.

Review symptom pattern against both major diagnostic frameworks. Assess what testing has been done, what's been done correctly, and what's still missing.

Integrate the case with co-occurring conditions — POTS, hEDS, GI dysmotility, autoimmune features — rather than treating mast-cell symptoms in isolation.

Map the treatment landscape — the H1/H2 framework, mediator-specific agents, stabilizers, low-dose naltrexone, trigger management — with evidence grading per strategy.

Identify MCAS-aware specialists. Frame expectations about wait times, testing prep, and what to bring to each first visit.

The nine-stage workflow, applied

How a MCAS case moves through our workflow.

Our nine-stage workflow is the same for every engagement. What changes per condition is the content at each stage — the records we pull, the signals we apply, the specialists we map, the pathways we evaluate. Below, how your case specifically would move through each stage.

Stage 01 · Days 0–2

Qualification

Fit screen focuses on multi-system symptom pattern, prior workup, and willingness to pursue structured evaluation — including correctly-timed biomarker testing if not already done.

Stage 02 · Days 3–7

Intake & data aggregation

Records pull emphasizes all prior mast-cell testing, allergy workup, GI workup, and autonomic testing. Symptom log and trigger history built across months.

Stage 03 · Days 7–9

Case structuring

Case schema populated. Symptom cluster coded across six domains. Trigger map built. Co-occurring condition features (POTS, hEDS, GI) captured.

Stage 04 · Days 9–12

Signal analysis

Ternary Signal Library for MCAS applied — symptom-cluster signals, biomarker-gap signals, trigger patterns, and triad overlap all weighted against your presentation.

Stage 05 · Days 10–14

Evidence retrieval

Literature scan across the Afrin/Molderings and Akin/Valent frameworks, recent treatment trials, and evolving biomarker protocols. Evidence Matrix updated with each engagement.

Stage 06 · Days 14–17

Pathway mapping

Pathway map built across diagnostic (correct biomarker testing, timed sample collection), medical (H1/H2/stabilizer framework, specific mediator agents, LDN), trigger management, and specialist referral. MCAS-aware clinicians mapped from our Specialist Graph.

Stage 07 · Days 17–20

Synthesis & plan construction

Interventions scored on the Ternary Method. Sequencing typically: baseline testing before starting medications that affect biomarkers; H1/H2 trial before stabilizers; trigger management in parallel.

Stage 08 · Days 20–25

Delivery & calibration

Findings call emphasizes the treatment-as-experiment framework — MCAS typically requires iteration, not a single prescription. Priorities and constraints captured.

Stage 09 · Days 25–55

Execution support

30 days of asynchronous follow-up through any medication trials, biomarker testing, and specialist appointments. Treatment response captured for the Outcomes Ledger.

Deliverables

What you receive.

—A written case synthesis against the main diagnostic frameworks
—Integration with co-occurring conditions (POTS, hEDS, GI, autoimmune)
—Evidence-graded treatment-option map
—A trigger and environment audit framework
—Specialist identification with MCAS-specific experience
—A written action plan and follow-up support as you implement it

Common questions — MCAS

What prospective MCAS clients ask most.

How do I know if I have MCAS versus something else?

This is one of the harder clarifying questions in complex disease, and depends on which diagnostic framework your clinician applies. We review your symptom pattern, testing, and treatment trials against both major frameworks (Afrin/Molderings consensus II; Akin/Valent), and surface where the evidence is strongest in each direction.

Do I need lab-confirmed elevated tryptase?

No. Serum tryptase is often normal in MCAS — elevated tryptase typically indicates systemic mastocytosis, a different entity. We use the broader mediator-testing framework (urinary N-methylhistamine, PGD2 metabolites, leukotriene E4) and assess whether prior testing was correctly timed and handled.

Will you recommend treatments I can try on my own?

Not directly — we are not a medical practice. We map the treatment landscape (H1/H2 framework, mast-cell stabilizers, mediator-specific agents, low-dose naltrexone, trigger management) with evidence grades per strategy. Your plan is a conversation with your MCAS-aware clinician, not a self-administration protocol.

Can you review a previous workup that was called 'normal'?

Yes, and we often find that 'normal' means the wrong tests were ordered, samples were mishandled, or baseline specimens were substituted for during-episode. A significant fraction of our MCAS work is re-evaluating prior workups for protocol errors.

How does MCAS relate to hEDS or POTS in my case?

The MCAS-POTS-hEDS triad is central to how we think about mast-cell presentations. If any of the three are suspected, our case structuring evaluates all three together rather than in isolation. Addressing MCAS often changes POTS treatment response and vice versa.

Ready for a case review?

Applications are reviewed within three business days.

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