Allergy and Hypersensitivity

Coverage Summary

This policy (Aetna Clinical Policy Bulletin Number 0038) defines medical necessity criteria and coverage limits for allergy and hypersensitivity testing and treatments, and lists tests/treatments considered experimental or investigational. It distinguishes covered procedures (e.g., percutaneous and intradermal skin testing, in vitro IgE testing, patch/photo testing, bronchial/exercise/ingestion challenge, SET for selected patients, allergy immunotherapy when criteria met) from non‑covered/experimental services (many unvalidated assays and novel immunotherapies).

Key program limits include an initial in vitro IgE screen of up to 40 inhalant tests or 12 food/other tests, typical maximum testing volumes of up to 70 percutaneous tests followed by up to 40 intracutaneous tests for inhalant evaluation, and SET (IDT) up to 14 titration tests (with an additional 40 antigens or 80 IDT injections potentially medically necessary if initial results are positive). Percutaneous CPT codes (e.g., 95004/95017/95018) are noted and are not covered after allergen immunotherapy unless criteria are met.

The policy includes operational and documentation requirements (medical history, exam, test results, treatment plan and injection records) and coding guidance (covered CPT/HCPCS and listed experimental codes). Policy administrative metadata: policy number 0038; Effective date 07/21/1995; Last review 02/08/2024; Next review listed as 01/11/2024.

Medical-Necessity Criteria

Medical Necessity - Allergy Testing (general)

Aetna considers specific allergy testing medically necessary for members with clinically significant allergic history of symptoms when ALL of the following criteria are met:

Symptoms are not adequately controlled by empiric conservative therapy; and

Testing must correlate specifically to the member's history, risk of exposure and physical findings; and

Test technique and/or allergens tested must have proven efficacy demonstrated through scientifically valid medical studies published in the peer-reviewed literature.

Epicutaneous (scratch, prick or puncture) testing

Epicutaneous (scratch, prick or puncture) testing is considered medically necessary when IgE-mediated reactions are suspected and testing matches the clinical history. Perform percutaneous testing for:

Foods

Hymenoptera (stinging insects)

Inhalants

Specific drugs (e.g., penicillins and macromolecular agents)

Intradermal (Intracutaneous) testing

Intradermal (intracutaneous) testing is considered medically necessary when IgE-mediated reactions are suspected for selected allergens and when percutaneous tests are negative or insufficient. Do not use intradermal testing for food allergy.

Hymenoptera venom allergy (stinging insects)

Inhalants

Specific drugs (e.g., penicillins and macromolecular agents)

Number limits - Epicutaneous and Intracutaneous

Typical number limits for skin testing (may vary by clinical need):

Evaluation of inhalant allergy may require up to 70 percutaneous (epicutaneous) tests.

Follow-up intracutaneous testing may include up to 40 intradermal tests (often performed when percutaneous tests are negative).

When determining starting dose for immunotherapy in highly allergic patients, up to 14 skin endpoint titration (SET) dilutional tests may be necessary; an additional 40 antigens or up to 80 IDT injections may be medically necessary if initial results are positive.

Skin Endpoint Titration (SET / IDT)

Skin Endpoint Titration (SET / IDT) — also called intradermal dilutional testing — is used to determine the starting dose for immunotherapy in highly allergic individuals.

Members highly allergic to hymenoptera venom (stinging insects).

Members highly allergic to inhalants.

When used to determine starting dose for immunotherapy, up to 14 titration tests may be necessary; if any initial titration test is positive, an additional 40 antigens or up to 80 IDT injections may be medically necessary.

SET is inappropriate as a substitute for standard skin testing; use only when needed to establish a safe starting concentration for immunotherapy.

Skin Patch Testing

Patch testing is considered medically necessary for diagnosing allergic contact dermatitis.

Skin patch testing for contact dermatitis (up to 80 units is considered medically necessary).

Photo Patch Testing and Photo Tests

Photo-patch testing and photo tests are used to evaluate photo-allergy and photosensitivity disorders.

Photo-patch testing for diagnosing photo-allergic contact dermatitis.

Phototests for evaluating photosensitivity disorders.

Bronchial Challenge Test

Bronchial challenge testing (e.g., methacholine, histamine, or antigen) is used to define asthma or airway hyperreactivity when indicated.

When bronchial challenge testing is being used to identify new allergens for which skin or blood testing has not been validated.

When skin testing is unreliable or cannot be performed.

Exercise Challenge Testing

Exercise challenge testing is medically necessary for diagnosis of exercise-induced bronchospasm.

Evaluation of exercise-induced bronchospasm (exercise challenge testing).

Ingestion (Oral) Challenge Test

Ingestion (oral) challenge testing is considered medically necessary for evaluation of suspected food or other non-drug reactions and for certain drug challenges when strict conditions are met.

Food or other substances (e.g., metabisulfite).

Drugs when ALL of the following are met:

History of allergy to the particular drug; and

There is no effective alternative drug; and

Treatment with that drug class is essential.

In Vitro IgE Antibody Tests

In vitro IgE antibody tests (e.g., RAST, MAST, FAST, ELISA, ImmunoCAP) are medically necessary in specific clinical scenarios and may be used as an initial screen in lieu of skin testing within limits.

Indications for in vitro testing: patients on skin-test–suppressive medications that cannot be discontinued; widespread skin disease (dermatographism, generalized eczema); uncooperative patients (small children, impaired individuals); history suggesting high anaphylaxis risk with skin testing; evaluating cross-reactivity between insect venoms; adjunctive testing for ABPA or certain parasitic diseases.

Initial allergy screen limits: up to 40 inhalant tests and up to 12 food/other tests. Additional tests may be medically necessary if any initial test is positive; if all initial tests are negative, further in vitro testing beyond the initial screen is not considered medically necessary.

Operational notes: use in vitro testing when skin testing is contraindicated or impractical (medication suppression, skin disease, patient inability). Ensure testing correlates with clinical history and document reasons why skin testing could not be performed.

Total Serum IgE

Total serum IgE measurement (e.g., PRIST, RIST) is used in specific diagnostic evaluations.

Diagnostic evaluation for known or suspected allergic bronchopulmonary aspergillosis (ABPA).

Evaluation for hyper IgE syndrome.

Lymphocyte Transformation Tests

Lymphocyte transformation tests have limited allergy indications but are useful for specific non-allergy diagnoses.

Medically necessary: evaluation of persons with sensitivity to beryllium.

Medically necessary: evaluation of congenital or acquired immunodeficiency diseases affecting cell-mediated immunity (examples: severe combined immunodeficiency, common variable immunodeficiency, X-linked hyper IgM, Nijmegen breakage syndrome, reticular dysgenesis, DiGeorge syndrome, Nezelof syndrome, Wiscott-Aldrich syndrome, ataxia telangiectasia, chronic mucocutaneous candidiasis).

Medically necessary: evaluation in thymoma or to predict allograft compatibility in transplant setting.

Experimental/investigational: lymphocyte transformation tests are considered experimental and investigational for evaluation of persons with allergies or other hypersensitivities (including metal allergy testing).

Alpha-Gal (Meat) Allergy Testing

Alpha-gal (galactose-alpha-1,3-galactose) IgE testing is medically necessary when clinical presentation after mammalian meat ingestion meets specified criteria.

Testing is medically necessary when EITHER of the following occur within 3–6 hours after ingestion of mammalian meat:

Urticaria, angioedema, or anaphylaxis.

Gastrointestinal symptoms (abdominal pain, diarrhea, vomiting) accompanied by presyncope or syncope.

Ara h 2 Testing for Peanut Allergy

Ara h 2 specific IgE testing is considered medically necessary when peanut allergy is suspected and can aid diagnostic evaluation.

Ara h 2 testing for persons with suspected peanut allergy.

Allergy Re-testing and Repeat Percutaneous Testing

Routine allergy re-testing and repeat percutaneous testing are limited.

Repeat percutaneous testing is allowed if new sensitivities emerge during or after allergen immunotherapy, or if the person has failed to respond to allergen immunotherapy.

Routine repeated percutaneous allergy testing for monitoring response to immunotherapy is considered not medically necessary.

Performance of Both Percutaneous and IgE RAST for Same Allergens

Performing both percutaneous (skin prick) testing and IgE serologic testing for the same allergens is generally not necessary.

Performance of both percutaneous allergy tests and IgE RAST tests (blood) for the same allergens is considered not medically necessary.

Allergy Immunotherapy (General)

Allergy immunotherapy (subcutaneous) is considered medically necessary for selected IgE-mediated conditions when specific criteria are met.

Covered indications include allergic (extrinsic) asthma, dust mite atopic dermatitis, Hymenoptera venom sensitivity, mold-induced allergic rhinitis, perennial rhinitis, seasonal allergic rhinitis or conjunctivitis.

Required conditions: member has severe seasonal or perennial IgE-dependent symptoms after natural exposure AND BOTH of the following are met: member has skin test and/or serologic evidence of IgE-mediated sensitivity to a potent extract of the allergen; and avoidance or pharmacologic therapy cannot control symptoms or causes unacceptable side effects. OR

Life-threatening IgE-mediated allergy to insect stings (bees, hornets, wasps, fire ants). OR

Hypersensitivity to allergens that cannot be managed by medication or avoidance.

Allergy immunotherapy is considered experimental and investigational for all other indications.

Rapid Desensitization (rush, cluster, acute)

Rapid desensitization (rush, cluster, acute) may be medically necessary in specific situations; preparations and premedication considerations apply.

Indications (ANY): allergy to a particular drug that cannot be treated effectively with alternative medications; insect sting hypersensitivity (hymenoptera); members with moderate to severe allergic rhinitis who need treatment during or immediately before the season.

Operational notes: allergens should be individually prepared for the patient and based on appropriate skin or in vitro testing. Rapid desensitization is considered experimental and investigational for other indications. If pregnancy is contemplated and initiation of immunotherapy is required, rapid desensitization is an acceptable approach.

Premedication and procedural notes: premedication regimens (antihistamines, corticosteroids) may be used per protocol to reduce reaction risk; specific premedication for RDD to paclitaxel and other agents should follow published clinical guidance and be documented in the medical record.

Epinephrine Kits

Epinephrine auto-injector kits are indicated to prevent or treat anaphylactic reactions in high-risk individuals.

Persons with a history of life-threatening reactions to insect stings, foods, drugs, or other allergens.

Individuals with severe asthma at risk for anaphylaxis.

Individuals who require epinephrine during immunotherapy.

Epinephrine kits are considered experimental and investigational for indications other than those listed above.

Experimental and Investigational - Tests and Procedures

Aetna considers many tests and procedures experimental and investigational for allergy evaluation when there is insufficient evidence of effectiveness.

Examples of tests/procedures considered experimental/investigational include (but are not limited to): ALCAT test, IgG4 and other unproven antibody or leukocyte activation assays for routine allergy diagnosis, commercial/novel unvalidated products (e.g., Allergenex, Alzair Allergy Blocker, MBG AlerjSTOP), autologous whole-blood or serum acupoint injection for chronic urticaria, ligelizumab for chronic spontaneous urticaria (investigational unless otherwise approved), skin patch testing for irritable bowel syndrome, intradermal testing to foods (not appropriate due to high false-positive rate and risk of anaphylaxis), intradermal grass pollen immunotherapy and other intradermal immunotherapy approaches that lack evidence, subcutaneous depot steroids or intramuscular depot steroids for allergic rhinitis, chemical cautery (silver nitrate) of nasal mucosa for allergic rhinitis, oral immunotherapy (OIT) for peanut allergy outside established protocols or clinical programs.

Operational note: Documentation in the medical record must support clinical indications, prior therapies tried, rationale for experimental/novel testing if used (including review of evidence and informed consent), and any prior authorization when required.

Clinical statements / guidance and Documentation requirements

Additional clinical and operational guidance and documentation requirements to support medical necessity and proper billing.

Documentation requirements: clearly document history of allergic symptoms, exposures, prior conservative therapy and response, physical findings, indication for specific test, and why alternative testing (or discontinuation of suppressive medications) is not feasible when applicable.

Clinical guidance summary: diagnostic cut-offs and interpretation should follow validated, peer-reviewed sources; use component-resolved diagnostics (e.g., Ara h 2) where evidence supports improved specificity for clinical decision-making.

Special populations/conditions: for food protein-induced enterocolitis syndrome (FPIES), diagnosis is primarily clinical and oral food challenge under controlled conditions may be required; skin testing and specific IgE testing are of limited value for typical FPIES.

Percutaneous testing after immunotherapy: repeat percutaneous testing is permitted for new sensitivities or lack of response to immunotherapy; routine percutaneous testing solely for monitoring immunotherapy response is not medically necessary.

Not Covered / Experimental Tests and Treatments

Coding

Covered CPT codes (when selection criteria met) - Percutaneous tests and relatedCPTCovered

95004	Percutaneous tests (scratch, puncture, prick) with allergenic extracts, immediate type reaction, including test interpretation and report by a physician, specify number of tests [not covered AFTER allergen immunotherapy]
95017	Allergy testing, any combination of percutaneous and intracutaneous, sequential and incremental, with venoms, immediate type reaction, including test interpretation and report, specify number of tests [not covered AFTER allergen immunotherapy]
95018	Allergy testing, any combination of percutaneous and intracutaneous, sequential and incremental, with drugs or biologicals, immediate type reaction, including test interpretation and report, specify number of tests [not covered AFTER allergen immunotherapy]

Covered CPT codes - IntradermalCPTCovered

95024	Intracutaneous (intradermal) tests with allergenic extracts, immediate type reaction, including test interpretation and report by a physician, specify number of tests
95027	Intradermal tests, sequential and incremental, with allergenic extracts for airborne allergens, immediate type reaction, including test interpretation and report by a physician, specify number of tests
95028	Intracutaneous (intradermal) tests with allergenic extracts, delayed type reaction, including reading, specify number of tests

Covered CPT codes - SETCPTCovered

95027

Intracutaneous (intradermal) sequential and incremental tests for airborne allergens (used for SET when criteria met)

Covered CPT codes - Patch/Photo tests/Photo patchCPTCovered

95044	Patch or application tests(s) (specify number of tests)
95052	Photo patch test(s) (specify number of tests)
95056	Photo tests

Covered CPT codes - Bronchial challenge and related pulmonary codesCPTCovered

95070	Inhalation bronchial challenge testing; with histamine, methacholine, or similar compounds
95071	Inhalation bronchial challenge testing with antigens or gases, specify
94150	Vital capacity, total (separate procedure)
94200	Maximum breathing capacity, maximum voluntary ventilation
94621	Pulmonary stress testing; complex
94680	Oxygen uptake, expired gas analysis; rest and exercise, direct, simple
94681	Including CO2 output, percentage oxygen extracted
94690	Rest, indirect (separate procedure)
94726	Plethysmography for determination of lung volumes and airway resistance
94729	Diffusing capacity

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1/2

Covered HCPCS codes - Bronchial challenge agentHCPCSCovered

J7674

Methacholine chloride administered as inhalation solution through a nebulizer, per 1 mg

Covered CPT codes - Exercise challenge testing and spirometryCPTCovered

94010	Spirometry, including graphic record, total and timed vital capacity, expiratory flow rate measurement(s)
94060	Bronchodilation responsiveness, spirometry pre- and post-bronchodilator
94070	Bronchospasm provocation evaluation, multiple spirometric determinations
94617	Exercise test for bronchospasm, including pre- and post-spirometry, ECG, and pulse oximetry
94618	Pulmonary stress testing (eg, 6-minute walk test), including measurement of heart rate, oximetry, and oxygen titration
96419	Exercise test for bronchospasm including pre- and post-spirometry and pulse oximetry; without ECG recording(s)

Covered CPT codes - Ingestion (Oral) ChallengeCPTCovered

95076	Ingestion challenge test; initial 120 minutes of testing
95079	Each additional 60 minutes of testing (add-on)

Covered CPT/HCPCS codes - In vitro IgE tests and specific codesmixedCovered

83516	Immunoassay for analyte other than infectious agent antibody or antigen, qualitative or semiquantitative; multiple step method
83518	Single step method (e.g., reagent strip)
83519	Immunoassay, analyte quantitative; by radiopharmaceutical technique (eg, RIA)
83520	Immunoassay, not otherwise specified
86003	Allergen specific IgE; quantitative or semi-quantitative, each allergen [covered up to 40 inhalant or 12 food/other tests]
86005	Qualitative, multi-allergen screen [covered up to 40 inhalant or 12 food/other tests]
86008	Allergen specific IgE; recombinant or purified component, each [covered up to 40 inhalant or 12 food/other tests]

Covered CPT code - Total Serum IgECPTCovered

82785

Gammaglobulin; IgE

Covered CPT code - Lymphocyte transformation (specific non-allergy indication)CPTCovered

86353

Lymphocyte transformation, mitogen or antigen induced blastogenesis (covered for beryllium sensitivity and certain immunodeficiency/transplant indications; not covered for in-vitro metal allergy testing)

Covered CPT codes - Allergy immunotherapy (professional services)CPTCovered

95115-95170	Professional services for allergen immunotherapy (except home administration) [not covered for intradermal grass pollen immunotherapy or intranasal immunotherapy; immunotherapy for tree nut allergy not FDA-approved]
95199	Unlisted code for allergen immunotherapy services

Covered HCPCS codes - EpinephrineHCPCSCovered

J0171	Injection, adrenalin, epinephrine, 0.1 mg
J0173	Injection, epinephrine (belcher) not therapeutically equivalent to J0171, 0.1 mg

Other HCPCS/CPT related (medical benefit) and ICD-10 covered codesmixedCovered

J2357	Injection, omalizumab, 5 mg (related CPB referenced)
ICD-10 J30.1-J30.9	Allergic rhinitis
ICD-10 L20.84	Intrinsic (allergic) eczema
ICD-10 L25.4	Unspecified contact dermatitis due to food in contact with skin
ICD-10 L27.2	Dermatitis due to ingested food
ICD-10 L50.0	Allergic urticaria
ICD-10 T50.995+	Adverse effect of other drugs, medicaments and biological substances

Not covered / Experimental CPT/HCPCS codes (examples listed)mixedExperimental

0165U	Peanut allergen-specific IgE and quantitative assessment of 64 epitopes using ELISA (VeriMAP Peanut Dx) - not covered
0178U	Peanut allergen-specific quantitative assessment of multiple epitopes using ELISA - not covered
82784	Gammaglobulin (immunoglobulin) IgA, IgD, IgG, IgM, each - listed not covered for some indications
82787	Immunoglobulin subclasses - not covered for IgG4 testing
86258	Gliadin (deamidated) antibody - listed not covered in mediator/cytotoxic testing section
86343	Leukocyte histamine release test (LHR) - listed not covered for routine allergy testing
95060	Ophthalmic mucous membrane tests - listed not covered
A7023	Mechanical allergen particle barrier/inhalation filter, cream, nasal, topical - HCPCS not covered

Neutral - No specific procedure codes providedmixed

No codes listed

Provider Actions and Operational Requirements

Prior Authorization

Selection criteria required for testing

Selection criteria required for allergy testing. Testing should only be performed when all three core selection criteria are met to ensure clinical relevance and evidence-based use of diagnostics.

Symptoms are not adequately controlled by empiric conservative therapy (uncontrolled symptoms).
Testing findings must correlate to the member's history, risk of exposure and physical findings.
Test technique and allergens tested must have proven efficacy demonstrated through peer-reviewed scientific studies (evidence-based diagnostic testing).

Documentation Required

Documentation requirements for testing and immunotherapy

Document specific clinical indications and required elements in the medical record for specialty tests and procedures. Maintain clear, contemporaneous documentation to support medical necessity, timing, and services billed.

Background and Evidence Summary

Background: The CPB summarizes evidence and clinical guidance across many domains. It affirms established diagnostic standards (skin testing and in‑vitro sIgE when indicated) and emphasizes that the oral food challenge (OFC) remains the diagnostic gold standard for IgE‑mediated food allergy. It also outlines settings where in‑vitro testing is preferred (e.g., patients on suppressive meds, widespread skin disease, uncooperative patients, risk of anaphylaxis) and repeats the initial in vitro screen limits of 40 inhalant / 12 food/other tests with additional testing allowed only if initial screen positive.

Evidence highlights: Sublingual immunotherapy (SLIT) has moderate evidence of efficacy for allergic rhinitis/asthma from multiple RCTs and systematic reviews (symptom and medication reductions), but heterogeneity and methodological issues remain; safety concerns include frequent local oral reactions and rare anaphylaxis reports (see SLIT systematic reviews and trials).

Oral immunotherapy (OIT) for food allergy increases desensitization rates but also substantially increases harms: the PACE meta-analysis found higher anaphylaxis risk (RR ~3.12), increased epinephrine use (RR ~2.21) and more serious adverse events; benefits versus harms are unclear.

Ara h 2 guidance: For suspected peanut allergy when a single diagnostic test is used, Ara h 2 component testing is suggested because it offers higher specificity (but lower sensitivity) compared with SPT or whole‑allergen sIgE.

Alpha‑gal (mammalian meat) evidence: Multiple observational studies support measuring alpha‑gal specific IgE in patients with delayed reactions (typically 3–6 hours after mammalian meat ingestion) presenting with urticaria/angioedema/anaphylaxis or GI symptoms with presyncope; skin tests with commercial meat extracts may be insensitive and sIgE is generally detectable.

Basophil Activation Test (BAT): Meta‑analytic data indicate BAT has relatively high specificity and good sensitivity as an adjunctive in immediate drug hypersensitivity and other settings (pooled sensitivity ~78%, specificity ~95%), but larger studies and standardization are needed and BAT is listed among tests considered experimental for routine allergy evaluation in this policy.

Definitions

Term	Definition
SET	Skin Endpoint Titration, also known as intradermal dilutional testing (IDT), used to determine starting dose for immunotherapy.
SCIT	Subcutaneous immunotherapy (allergy shots) involving repeated administration of specific allergens by injection.
SLIT	Sublingual immunotherapy involving administration of allergen extracts under the tongue.
MRT	Mediator Release Test—measures aggregate release of inflammatory mediators from leukocytes after exposure to foods/additives.
EPD / LDA	Enzyme potentiated desensitization / Low dose allergens—non‑FDA‑approved immunotherapy approaches using enzyme‑enhanced small allergen doses.
Alpha-gal (galactose-α-1,3-galactose)	A carbohydrate epitope in non‑primate mammalian meats associated with delayed IgE‑mediated allergic reactions.
Chronic Urticaria (CU) Index	A basophil‑activation based assay to detect functional autoantibodies associated with chronic idiopathic urticaria.
BAT	Basophil activation test — in‑vitro functional assay measuring basophil activation markers (e.g., CD63, CD203c) upon allergen/drug stimulation.
LTT	Lymphocyte transformation test — in‑vitro test for metal allergy assessing lymphocyte proliferation; clinical utility for implant decisions is unproven.
OIT	Oral immunotherapy — controlled exposure to food allergens aiming to induce desensitization or tolerance.
FPIES	Food protein-induced enterocolitis syndrome — non‑IgE-mediated food allergy causing GI symptoms.
sIgE	Serum food-specific immunoglobulin E testing.
OFC	Oral food challenge - the gold standard test for diagnosis of IgE‑mediated food allergy.
SPT	Skin prick test.
PbP	Prick by prick testing.
Ara h 2	Peanut component (Ara h 2) component‑resolved diagnostic; suggested when a single diagnostic test is used—higher specificity but lower sensitivity than SPT/sIgE.
Mediator Release Test (MRT)	See MRT — measures aggregate mediator release; manufacturer claims unvalidated; considered experimental/investigational.
sIgE (specific immunoglobulin E)	Specific immunoglobulin E.

Evidence	Key point / result
SLIT systematic review (Lin et al 2013)	63 RCTs (n=5,131): moderate evidence SLIT improves asthma and rhino‑conjunctivitis symptoms, reduces medication use; local reactions frequent, anaphylaxis not reported in review
SLIT Cochrane review (Calderon et al 2011)	42 trials (n=3,958): SLIT reduced ocular symptom scores and some individual symptoms; heterogeneity and quality concerns
House dust mite SLIT RCT (Virchow et al, 2016)	Reduced risk of moderate/severe asthma exacerbation during ICS reduction: HR 0.72 (6 SQ‑HDM) and 0.69 (12 SQ‑HDM); AEs mainly mild‑to‑moderate oral symptoms
OIT PACE harms (Chu et al, 2019)	Peanut OIT increases desensitization but also increases anaphylaxis (RR 3.12), epinephrine use (RR 2.21), and serious AEs; benefits vs harms unclear
Ara h 2 guidance (AAAAI 2020)	Ara h 2 suggested when a single diagnostic test is used — greater specificity but lower sensitivity than SPT or sIgE
Alpha‑gal observational evidence (multiple studies, e.g., Wilson 2019, Mullins 2012)	Alpha‑gal specific IgE detectable in most affected patients; delayed reactions typically 2–6 hours after mammalian meat ingestion; useful diagnostic marker when history fits
Basophil activation test meta‑analysis (Cuervo‑Perez et al, 2014)	BAT sensitivity ~78% (95% CI 74–81), specificity ~95% (95% CI 83–100); sIgE sensitivity ~72%, specificity ~90% — BAT is a useful adjunct but protocols need standardization
Chronic Urticaria (CU) Index studies (Viswanathan et al 2012; Cho et al 2013)	CU Index associated with refractory CIU (odds ratio ~4.5 in one retrospective study) but clinical utility and standardization limited
Depot steroid risks (Aasbjerg et al, 2013)	Retrospective registry study associated depot steroid injections for rhinitis with increased risk of diabetes (RR 1.5) and osteoporosis (RR 1.2); recommendation to avoid depot steroids for rhinitis
Intradermal grass pollen RCT (Slovick et al, 2017)	No clinical efficacy; intradermal therapy associated with worse nasal and asthma symptoms and immunologic priming — not recommended
Ligelizumab phase II (Maurer et al, 2019)	Dose‑finding RCT: 72 mg and 240 mg showed higher rates of complete control at week 12 versus omalizumab and placebo; needs phase III confirmation
SLIT safety/pediatric evidence summaries (various systematic reviews/meta‑analyses)	Overall SLIT evidence mixed; moderate support for efficacy but heterogeneity and methodological issues; pediatric evidence insufficiently robust
Epicutaneous/in vitro testing and component diagnostics (background evidence)	Component testing (eg, Ara h 2) promising for peanut; many novel molecular/epitope assays under study but not yet universally adopted for routine use

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