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Para conocer los horarios, visitas sin turno y citas.Acetylcholine Receptor (AChR)-binding Antibodies; Acetylcholine Receptor (AChR)-blocking Antibodies; Acetylcholine Receptor (AChR)-modulating Antibodies; Striational Antibodies.
Reflex criteria: If Acetylcholine Receptor (AChR)-binding and blocking are normal, will reflex to Muscle Specific Kinase (MuSK) Antibodies.
This assay currently is not available in New York state.
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This assay currently is not available in New York state. |
6 - 8 days
Turnaround time is defined as the usual number of days from the date of pickup of a specimen for testing to when the result is released to the ordering provider. In some cases, additional time should be allowed for additional confirmatory or additional reflex tests. Testing schedules may vary.
Serum
4 mL divided into two tubes
2 mL (Note: This volume does not allow for repeat testing.)
Red-top tube or gel-barrier tube
Allow a minimum clotting time of 30 to 60 minutes with serum separation within 2 hours of collection. Send serum samples in plastic transport tubes.
Refrigerate.
Temperature | Period |
---|---|
Room temperature | 7 days (stability provided by manufacturer or literature reference) |
Refrigerated | 14 days (stability provided by manufacturer or literature reference) |
Frozen | 14 days (stability provided by manufacturer or literature reference) |
Freeze/thaw cycles | Stable x3 (stability provided by manufacturer or literature reference) |
No isotopes administered 24 hours prior to venipuncture.
Excessive hemolysis; chylous serum; recently administered radioisotopes; plasma specimen
Tests for the laboratory diagnosis of myasthenia gravis (MG)
In rare cases AChR antibodies can be found in patients with other autoimmune disorders or with thymoma without MG.1
The causative autoantibody cannot be identified in up to 10 percent of patients with MG.
This test was developed and its performance characteristics determined by Labcorp. It has not been cleared or approved by the Food and Drug Administration.
See individual tests.
Myasthenia gravis (MG) is an acquired disorder of neuromuscular transmission that is characterized by skeletal muscle weakness and fatigability on exertion that is exacerbated by repeated muscle activity.2-7 This autoimmune disease is caused by antibodies directed toward receptors embedded in the motor endplate of the neuromuscular junction. Progressive weakness of the ocular muscles manifesting as asymmetric ptosis and variable diplopia are the presenting symptoms in 60% of patients.5,7 Many patients progress to more generalized weakness of peripheral limb muscles and muscles required for body posture, including facial and neck muscles. Bulbar muscle weakness compromises speaking (dysarthria), chewing and swallowing (dysphagia) and respiratory muscle weakness can lead to a myasthenic crisis where patients need to be ventilated artificially.8 Clinical symptoms may be restricted to one muscle group, in particular the eye muscles (ocular MG), or may become generalized (generalized MG).5-8
Patients with MG frequently have thymic abnormalities (thymic hyperplasia or thymoma).9 Ten to 15 percent of patients with MG patients have thymoma, and up to 50% of thymoma patients develop MG.9 It is thought that the thymus plays a role in MG pathogenesis and these patients respond well to the surgical removal of the thymus gland.10
Neonatal MG can occur as a result of trans-placental transit of antibodies from an affected mother to the fetus, or in some cases, due to antibody to the fetal form of AChR.11-13 In the latter case, the mother may be unaffected. It should be noted that the AChR antibody assays employed by Labcorp contain a mixture of adult and embryonic AChRs allowing for the detection of autoantibodies to both proteins. In most cases affected babies are born with a diminished ability to suck and generalized hypotonia. Decrease in utero feta movement caused by MG can also result in arthrogryposis multiplex congenital, a condition where the neonate suffers from contractures in more than two joints and in multiple body areas.
The majority of patients with MG have antibodies to the acetylcholine receptor (AChR) and, less frequently, to the other proteins at postsynaptic membrane of the neuromuscular junction.14-16 AChR antibodies impede neuromuscular transmission by a range of pathogenic mechanisms including the alteration of tissue architecture and/or by causing a reduction the density of functionality of AChRs.1,17-21 Three functionally different types of antibodies against muscle AChR can be measured.1,21-24
• AChR binding antibodies attach to the AChR activate the complement system result in destruction and focal lysis of the neuromuscular junction leading to the destruction of AChR and AChR-related protein at the end-plate.1,20
• AChR blocking antibodies functionally block the binding of the neurotransmitter acetylcholine to the receptor.20 These antibodies usually occur in association with AChR-binding antibodies and have a higher prevalence in generalized MG compared with ocular MG.20
• AChR modulation antibodies crosslink receptor subunits in such as way as to cause the receptors to be internalized and degraded in a process known as antigenic modulation.20,22,25-27 Modulating antibodies are implicated with an increased risk of thymoma and the majority of patients with thymoma have modulating antibodies.28
Tests for serum autoantibodies are highly sensitive and specific for generalized MG but lack sensitivity when there is pure ocular involvement.1,14,29-30 Approximately 85% of patients with generalized MG have detectable muscle AChR antibodies (of one or more types), while fewer patients with ocular MH have the antibodies (50-60%).4,30 In general, an elevated level of any one of the AChR-binding antibodies in a patient with compatible clinical features confirms the diagnosis of MG. Approximately 15% of individuals with confirmed myasthenia gravis have no measurable AChR binding, blocking, or modulating antibodies. Thirty-five percent of these patients (six percent of all MG patients) will have antibodies directed against a muscle-specific tyrosine kinase (MuSK).10,31 Autoantibodies levels do not generally correlate with disease severity. However, in individual patients, serial antibody titers tend to correlate with disease status.18,19,32-34
Autoantibodies directed against the contractile elements of striated muscle are found in 30% of adult patients with myasthenia gravis and in 80% of those with thymoma.35-37 Striational antibodies are associated with the late-onset MG subgroup and are rarely found in AChR antibody-negative MG.
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