Diagnosis of antiphospholipid syndrome is often made through the combination of symptoms and testing. Repeat antibody testing 12 weeks after discovering the presence of antiphospholipid antibodies (aPL) is needed to establish a diagnosis because false positives can occur. While APS was previously categorized into primary and secondary APS based on the absence or presence of concurrent autoimmune disease respectively, the 16th International Congress on Antiphospholipid Antibodies Task Force categorizes APS into 6 categories: were replaced by the Sydney criteria in 2006. • Blood clot in three or more organs or tissues
and • Development of manifestations simultaneously or in less than a week
and • Evidence of small vessel blood clot in at least one organ or tissue
and • Laboratory confirmation of the presence of aPL.
Lab testing Antiphospholipid antibody tests are either liquid-phase coagulation
assays to detect
lupus anticoagulant or solid phase
ELISA (enzyme-linked immunosorbent assay) to detect
anti-cardiolipin antibodies and
β2 glycoprotein 1. The use of testing for antibodies specific for individual targets of aPL such as
phosphatidylserine is currently under debate.
Lupus anticoagulant This is tested for by using two coagulation tests that are phospholipid-sensitive, due to the heterogeneous nature of the
lupus anticoagulant antibodies. A patient with lupus anticoagulant antibodies on initial screening will typically have been found to have a prolonged
partial thromboplastin time (PTT) that does not correct in an 80:20 mixture with normal human
plasma (50:50 mixes with normal plasma are insensitive to all but the highest antibody levels). The PTT (plus 80:20 mix),
dilute Russell's viper venom time, silica clotting time and
prothrombin time (using a lupus-sensitive
thromboplastin) are the principal tests used for the detection of
lupus anticoagulant. The Scientific and Standardization Committee for lupus anticoagulant/antiphospholipid antibodies of the International Society on Thrombosis and Haemostasis no longer recommends the
kaolin clotting time, dilute thromboplastin time, and Taipan/Ecarin snake venom based assays due to implementation issues from a variety of factors. Distinguishing a lupus anticoagulant antibody from a specific coagulation factor inhibitor (e.g.:
factor VIII) is normally achieved by differentiating the effects of a lupus anticoagulant on factor assays from the effects of a specific coagulation factor antibody. The lupus anticoagulant will inhibit all the contact activation pathway factors (
factor VIII,
factor IX,
factor XI and
factor XII). Lupus anticoagulant will also rarely cause a factor assay to give a result lower than 35 iu/dl (35%) whereas a specific factor antibody will rarely give a result higher than 10 iu/dl (10%). Monitoring IV anticoagulant therapy by the PTT ratio is compromised due to the effects of the lupus anticoagulant and in these situations is generally best performed using a chromogenic assay based on the inhibition of
factor Xa by
antithrombin in the presence of
heparin.
Anticardiolipin and β2glycoprotein 1 antibodies Anti-cardiolipin antibodies can be detected using an
enzyme-linked immunosorbent assay (ELISA)
immunological test, which screens for the presence of β2glycoprotein 1 dependent anticardiolipin antibodies. A
low platelet count and positivity for antibodies against
phosphatidylserine may also be observed in a positive diagnosis.
False results The presence of antiphospholipid antibodies may not indicate APS, which is why considering the symptoms present and retesting antibody levels is essential. People may be transiently positive, incorrectly positive, or incorrectly negative if they are tested when the following is occurring: • infection • pregnancy • blood clot • states in which
acute-phase proteins, bilirubin, or fats are elevated •
anticoagulation (i.e.
warfarin,
heparin) It is recommended to generally re-test people 12 weeks after the first positive test to confirm that it was correct, except for those who test positive during pregnancy. For that group, it is recommend to wait 3 months to re-test if possible. Re-testing is more nuanced if the person is taking an anticoagulant, which may require not taking the medication for a certain period of time or specifically timing the test. Also, patients who have certain antiphospholipid antibodies may have false positive
VDRL test, which aims to detect a
syphilis infection. This occurs because the aPL bind to the lipids in the test and make it come out positive. A more specific test for syphilis,
FTA-Abs, will not have a false-positive result in the presence of aPL.
Differential diagnosis For people with blood clot related APS, other conditions that can cause blood clots should be considered including but not limited to acquired
blood clots, genetic
thrombophilia, and
paroxysmal nocturnal hemoglobinuria. Genetic thrombophilia can coexist in some patients with APS. For people with pregnancy related APS, other causes of
recurrent miscarriage should be considered before the diagnosis of APS, such as genetic, structural, or immune abnormalities. ==Treatment==