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HelpTest Code C2NAD PrecivityAD, Plasma
Ordering Guidance
This blood test is intended for use in patients aged 55 and older with signs or symptoms of mild cognitive impairment or dementia who are undergoing evaluation for Alzheimer disease or other forms of cognitive decline.
Shipping Instructions
1. Specimen should be shipped frozen on dry ice
2. Place labeled aliquot tube inside a larger tube or vial for transport.
Specimen Required
Supplies: Screw cap micro tube, 2 mL, PCR Performance Tested, Low protein-binding (T983)
Collection Container/Tube: 10 mL Purple top (K EDTA)
Submission Container/Tube: 2-mL screw cap micro tubes
Specimen Volume: 1.5 mL
Collection Instructions:
1. Centrifuge within two hours of collection.
2. Aliquot plasma into a 2 mL micro tube.
3. Freeze plasma (no longer than 2 hours after collection) at -20° C or below.
Useful For
Assisting in the evaluation of adult patients, aged 55 years and older, with signs or symptoms of mild cognitive impairment or dementia who are being assessed for Alzheimer disease and other causes of cognitive decline
This is not intended for patients younger than 55 years, or for use as a screening test in patients without signs or symptoms of cognitive impairment, or for serial testing for assessment of longitudinal changes.
Method Name
Immunoprecipitation/Liquid Chromatography Tandem Mass Spectrometry (LC-MS/MS)
Reporting Name
PrecivityADSpecimen Type
PlasmaSpecimen Minimum Volume
1 mL
Specimen Stability Information
| Specimen Type | Temperature | Time | Special Container |
|---|---|---|---|
| Plasma | Frozen | ||
Reject Due To
| Gross hemolysis | Reject |
| Gross lipemia | Reject |
| Gross icterus | Reject |
| Outside of age range Specimen collected outside of testing range (too long in storage before arrival to testing facility) Insufficient volume Incorrect labeling |
Reject |
Clinical Information
Alzheimer disease (AD) is defined pathologically by the presence of amyloid plaques and neurofibrillary tangles in the brain. Clinical characteristics include gradual onset of mild cognitive impairment (MCI), behavioral changes such as apathy, withdrawal, or agitation, and disease progression to middle and later stage dementia.(1,2) Currently, no test detects AD with 100% accuracy; definitive diagnosis occurs at brain autopsy.
MCI impacts 12% to 18% of people in the United States over age 60 and is often an initial clinical sign of AD.(3) Detection of AD at an early stage, such as at onset of MCI or memory loss, can optimize medical management by providing access to therapies and clinical trials and by allowing for lifestyle changes that prioritize aerobic exercise, quality sleep and a healthy diet. Detection at first signs of MCI is also important for personal or family knowledge and planning, and for accessing appropriate community support and resources. Exclusion of AD with a high degree of certainty is equally important since MCI can have other etiologies, some of which are treatable.
Amyloid positron emission tomography (PET) scan and cerebrospinal fluid (CSF) testing detect brain amyloid pathology with high sensitivity and specificity in patients with MCI and early dementia.(4,5) Results of these tests are interpreted in the context of the patient’s clinical findings and other clinical work-up, as the neuropathological changes associated with AD can be seen in unaffected individuals.(4,5) Highly sensitive and specific blood biomarker testing offers an accessible and less procedurally complex option to amyloid PET scan or CSF testing for assessment of brain amyloid plaques.(6,7)
The PrecivityAD test is an analytically and clinically validated blood test that aids healthcare providers in the diagnosis of AD in patients with MCI and early-stage dementia. This evaluation simultaneously quantifies plasma amyloid beta (Abeta) 42 and 40 (Abeta42 and Abeta40) concentrations and determines the presence of apolipoprotein E (ApoE)-specific peptides (to determine APOE genotype). The test’s statistical algorithm combines the Abeta 42/40 ratio, established APOE genotype, and patient age to calculate the likelihood that a patient is positive for the presence of amyloid plaques by amyloid PET scan.(6-8) APOE proteotype/genotype, included in the test results, can aid in decision-making about treatment paths for some patients: In recent clinical trials for amyloid-reducing therapies, the E4 allele showed association with development of amyloid-related imaging abnormalities (ARIA); cerebral edema (ARIA-E); and cerebral microhemorrhages (ARIA-H).(9,10)
Reference Values
Amyloid Probability Score (APS): 0-100
Low (0-35): Consistent with absence of amyloid plaques
Intermediate (36-57)
High (58- 100): Consistent with presence of amyloid plaques
Abeta42/40 Ratio
≥0.095: Consistent with absence of amyloid plaques
ApoE Proteotype
E2/E2, E2/E3, E2/E4, E3/E3, E3/E4, E4/E4
-E3 is the most common allele.
-E4 allele is associated with increased risk of amyloid plaques.
-E2 allele is associated with lower risk of amyloid plaques.
Interpretation
The Amyloid Probability Score (APS) represents the estimated likelihood from 0 (low likelihood) to 100 (high likelihood) that the patient is currently positive on amyloid positron emission tomography (PET) imaging (presence of amyloid plaques) based on their amyloid beta (Abeta) 42/40 ratio, age, and established APOE genotype.
A low APS result (0-35) is consistent with a negative amyloid PET scan result and, thus, a low likelihood of amyloid plaques. Absence of amyloid plaques is inconsistent with an Alzheimer disease diagnosis and indicates other causes of cognitive symptoms should be investigated.
An intermediate APS result (36-57) does not distinguish between the presence or absence of amyloid plaques and indicates further diagnostic evaluation may be needed to assess the underlying causes for the patient's cognitive symptoms.
A high APS result (58-100) is consistent with a positive amyloid PET scan result and, thus, a high likelihood of amyloid plaques. Presence of amyloid plaques is consistent with an Alzheimer disease diagnosis in someone who has cognitive decline, but alone is insufficient for a final diagnosis; clinical presentation and other factors should be considered along with the APS result.
Day(s) Performed
Monday through Friday
Report Available
10 days post sample receipt from MCL.Specimen Retention Time
60 daysPerforming Laboratory
C2N Diagnostics LLCTest Classification
C2N Diagnostics has developed and determined the analytical and clinical validity performance characteristics of this Laboratory Developed Test (LDT). This assay has been validated pursuant to CLIA regulations and is used for clinical purposes. This assay has not been cleared or approved by the FDA.CPT Code Information
0412U
LOINC Code Information
| Test ID | Test Order Name | Order LOINC Value |
|---|---|---|
| C2NAD | PrecivityAD | Not Provided |
| Result ID | Test Result Name | Result LOINC Value |
|---|---|---|
| ND2B | Amyloid Probability Score (APS) | Not Provided |
| ND2BF | APS Result | Not Provided |
| ND2C | Interpretation | Not Provided |
| ND2D | APS Reference Interval | Not Provided |
| ND2E | Patient Age | Not Provided |
| ND2F | Abeta42/40 Ratio | Not Provided |
| ND2G | Abeta42/40 Ratio Reference Interval | Not Provided |
| ND2H | Abeta42/40 Ratio Description | Not Provided |
| ND2I | ApoE Proteotype | Not Provided |
| ND2J | ApoE Proteotype Reference Interval | Not Provided |
| ND2K | Test Description | Not Provided |
| ND2L | Limitations of Test Result | Not Provided |
| ND2M | Methods and Assay Category | Not Provided |
| ND2N | References | Not Provided |
| ND2O | Report Comment | Not Provided |
| ND2P | Performing Site | Not Provided |
Forms
If not ordering electronically, complete, print, and send a Neurology Specialty Testing Client Test Request (T732) with the specimen.