The Antiphospholipid Antibody Panel: What Every NP Needs to Know (and the Pitfalls That'll Bite You) Unexplained clots, pregnancy losses, and a lab panel that's trickier than it looks.

 

The Antiphospholipid Antibody Panel: What Every NP Needs to Know (and the Pitfalls That'll Bite You)

Unexplained clots, pregnancy losses, and a lab panel that's trickier than it looks.

Antiphospholipid syndrome (APS) is one of those diagnoses that's simultaneously under-recognized and over-tested. In primary care, we see the patients who present with the red flags—unexplained DVT in a 30-year-old, recurrent pregnancy losses, a stroke in someone who "shouldn't" be having one. But the lab panel itself is full of pitfalls that can lead to misdiagnosis in both directions.

Let's walk through this one together.

What Is APS, in Plain English?

APS is an autoimmune disorder where the body produces antibodies against phospholipid-binding proteins. Despite the name "antiphospholipid" (which sounds like it should cause bleeding), these antibodies paradoxically cause clotting—both venous and arterial—plus pregnancy complications. APS can occur alone (primary APS) or in association with another autoimmune disease, most commonly SLE (secondary APS).

The Three Tests You Need to Know

The antiphospholipid antibody panel consists of three categories of tests. All three should be ordered together.

1

Lupus Anticoagulant (LA)
A functional coagulation assay (not an antibody level). Detected using phospholipid-dependent clotting tests, typically dRVVT (diluted Russell's viper venom time) and a sensitive aPTT. Despite the name, it's not specific to lupus, and despite being called an "anticoagulant," it causes clotting in vivo. The name is purely historical. LA is the single strongest predictor of thrombotic events.

2

Anticardiolipin Antibodies (aCL)
Measured as IgG and IgM isotypes by ELISA. Only moderate-to-high titers are clinically meaningful (generally >40 GPL/MPL, or >99th percentile per the lab). Low-positive titers are common in the general population, in infections, and in the elderly—they usually don't indicate APS. IgG isotype carries higher clinical risk than IgM.

3

Anti-β2-Glycoprotein I Antibodies (aβ2GPI)
Also measured as IgG and IgM by ELISA. β2GPI is the actual protein target of most pathogenic antiphospholipid antibodies. Like aCL, only moderate-to-high titers matter. This test adds diagnostic sensitivity—some patients with APS are positive for aβ2GPI but negative for aCL.

The Risk Hierarchy: Single, Double, and Triple Positive

Not all positive aPL profiles carry the same risk. This is critical for counseling patients and deciding management intensity:

aPL Profile	Risk Level	Clinical Implication
Triple positive (LA + aCL + aβ2GPI)	Highest risk	Strongest association with thrombosis and pregnancy morbidity. Often warrants lifelong anticoagulation after a thrombotic event.
Double positive (any two of three)	High risk	Significant clinical risk. Management depends on clinical context.
Single positive (one test only)	Lower risk	Especially if low-titer aCL or aβ2GPI only. May not represent true APS. Always confirm with repeat testing.
Isolated low-titer IgM (aCL or aβ2GPI)	Uncertain	Frequently non-specific. Can be seen with infections, medications, and aging. Rarely clinically significant alone.

The Pitfalls: This Is Where It Gets Messy

1. The 12-Week Confirmatory Rule

This is the single most important rule in APS testing: a positive aPL test must be confirmed with a repeat test at least 12 weeks later. Transient aPL positivity is extremely common—it occurs with infections (especially viral, including COVID-19), medications, and inflammatory states. A single positive test is NOT diagnostic. Per the 2023 ACR/EULAR classification criteria, the positive aPL test must occur within 3 years of the clinical event.

Critical Pitfall

Do NOT diagnose APS or start lifelong anticoagulation based on a single positive aPL panel. Always repeat at ≥12 weeks. Transient positivity after infections (including COVID-19, EBV, and other viral illnesses) is very common and does not equal APS.

2. Lupus Anticoagulant + Anticoagulation = Testing Nightmare

Here's the catch-22: most patients being tested for APS after a clot are already on anticoagulation. But LA testing is based on clotting-time assays, which are directly affected by:

• Heparin/LMWH — can cause false-positive LA results
• Warfarin — prolongs clotting times, making LA interpretation unreliable
• DOACs (direct oral anticoagulants) — particularly problematic; rivaroxaban and apixaban interfere with dRVVT and can cause false-positive LA results

Practical Tip

If LA testing is needed in an anticoagulated patient, discuss timing with your hematologist. Some labs offer DOAC-neutralizing agents (like DOAC-Stop) to mitigate interference, but this isn't universally available. aCL and aβ2GPI are not affected by anticoagulation—these solid-phase immunoassays can be drawn at any time.

3. "Classification Criteria" ≠ "Diagnostic Criteria"

This is a nuance that trips up a lot of clinicians. The 2023 ACR/EULAR APS classification criteria were designed for research standardization, not clinical diagnosis. They are highly specific (99%) but less sensitive (84%). In clinical practice, your judgment matters: a patient with classic livedo racemosa, pregnancy losses, and moderate-titer aCL may have APS even if they don't meet every classification criterion. Conversely, a single low-positive aCL in an elderly patient with a DVT and multiple traditional risk factors probably isn't APS.

4. Infections Can Trigger Transient aPL

This became glaringly obvious during COVID-19. Multiple studies showed that nearly half of hospitalized COVID patients had positive aPL results. These were overwhelmingly transient and did NOT carry the same thrombotic risk as true APS. Other infections that commonly trigger aPL include HCV, HIV, EBV, syphilis, and Lyme disease. The lesson: always repeat at 12 weeks, and always consider the clinical context.

5. False-Positive Syphilis Testing

The VDRL and RPR tests for syphilis use cardiolipin as an antigen. Patients with anticardiolipin antibodies can therefore have a biologically false-positive syphilis test. If your patient has a positive RPR but a negative treponemal test (FTA-ABS or TP-PA), consider aPL as the explanation—especially in a patient with SLE or suspected APS.

6. Low-Titer Positives Are Usually Noise

Low-positive aCL or aβ2GPI (between the 95th and 99th percentile) are common in the general population and rarely clinically significant for thrombotic APS. The 2023 classification criteria only count moderate-to-high titers. An exception: in obstetric APS, some experts consider persistent low-titer positivity clinically relevant, particularly if other risk factors are present.

When Should NPs Order This Panel?

Test When You See

• Unprovoked venous thromboembolism, especially in patients <50
• Arterial thrombosis in a young patient (stroke, MI) without traditional risk factors
• Recurrent pregnancy losses (≥3 before 10 weeks, or ≥1 at/after 10 weeks with normal fetal morphology)
• Preeclampsia or placental insufficiency before 34 weeks
• Unexplained thrombocytopenia (especially in an SLE patient)
• Livedo racemosa (lace-like purplish skin mottling)
• An SLE patient with any thrombotic event or pregnancy complication
• Biologically false-positive syphilis test (positive RPR, negative treponemal)

Do NOT Test

• As a routine screen in asymptomatic patients
• For a single provoked DVT with clear risk factors (post-surgical, immobilization, OCP use)
• As a "just in case" add-on to an ANA panel
• In the acute setting of an infection (wait until it's resolved and repeat at 12 weeks)

The 2023 ACR/EULAR Criteria: What Changed

The updated classification system introduced a weighted scoring approach across six clinical domains (macrovascular VTE, macrovascular arterial thrombosis, microvascular, obstetric, cardiac valve, and hematologic) and two laboratory domains (LA and solid-phase aCL/aβ2GPI assays). Patients need at least 3 points in both clinical AND laboratory domains to be classified as APS. The key takeaway for primary care: the bar for classification is now higher and more specific, which means fewer false-positive classifications but also a reminder that clinical diagnosis may still apply even when the scoring threshold isn't met.

Quick-Reference: The aPL Panel at a Glance

Test	Method	Key Pitfall	Affected by Anticoagulation?
Lupus Anticoagulant	Functional clotting assay (dRVVT, sensitive aPTT)	Strongest predictor, but affected by nearly all anticoagulants	Yes — heparin, warfarin, DOACs all interfere
Anticardiolipin (IgG/IgM)	ELISA immunoassay	Low titers are usually non-specific; IgG more significant than IgM	No
Anti-β2GPI (IgG/IgM)	ELISA immunoassay	Adds sensitivity; some APS patients are positive only for this	No

Bottom Line

APS is a real, serious, and treatable condition. But the lab panel is more nuanced than most providers realize. The three cardinal rules: always order all three tests together, always confirm at 12 weeks, and always interpret in clinical context. A single low-positive result on one test in an elderly patient after a provoked DVT is not the same as triple positivity in a 28-year-old with two unexplained pregnancy losses.

Know when to test, know when to wait, and know when to refer. Your hematologist and rheumatologist will thank you for sending them a patient with a properly collected, properly timed, complete panel rather than a single random aCL drawn during an acute COVID hospitalization.

Stay sharp out there.