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Test ID MGT1 Myasthenia Gravis (MG) Evaluation, Thymoma

Useful For

Investigating patients with suspected or proven thymoma, whether or not symptoms or signs of myasthenia gravis (MG) are present

 

Serially monitoring patients for recurrence or metastasis after removal of thymoma

 

Providing a quantitative autoantibody baseline for future comparisons in monitoring a patient's clinical course and the response to thymectomy and immunomodulatory treatment

 

Assessing the likelihood of occult thymoma in a patient with an acquired disorder of neuromuscular or autonomic transmission

 

Evaluating bone marrow transplant recipients with suspected graft-versus-host disease, particularly if there is evidence of weakness

 

Confirming that a recently acquired neurological disorder has an autoimmune basis (eg, MG or dysautonomia)

Profile Information

Test ID Reporting Name Available Separately Always Performed
ARBI ACh Receptor (Muscle) Binding Ab Yes Yes
STR Striational (Striated Muscle) Ab, S Yes Yes
ARMO ACh Receptor (Muscle) Modulating Ab No Yes
GANG AChR Ganglionic Neuronal Ab, S No Yes
GD65C GAD65 Ab Assay, CSF Yes Yes
VGKC Neuronal (V-G) K+ Channel Ab, S No Yes
CRMWS CRMP-5-IgG Western Blot, S Yes Yes
MGETI MG Thymoma Interpretation, S No Yes

Testing Algorithm

Recommended for investigation of: 1) a patient with suspected or proven thymoma, whether or not symptoms or signs of myasthenia gravis (MG) are present (also of value for serially monitoring patients after removal of thymoma; a rising autoantibody titer may herald tumor persistence or recurrence), or emergence of an unrelated neoplasm and 2) a bone marrow transplant recipient with suspected graft-versus-host disease, particularly if there is evidence of weakness.

 

See Myasthenia Gravis: Thymoma Diagnostic Algorithm in Special Instructions.

Method Name

ARBI, ARMO, GANG, GD65S, VGKC: Radioimmunoassay (RIA)

STR: Enzyme Immunoassay (EIA)

CRMWS: Western Blot

Reporting Name

MG Evaluation, Thymoma

Specimen Type

Serum

Container/Tube: 

Preferred: Red top

Acceptable: Serum gel

Specimen Volume: 3 mL

Additional Information: Patient should have no general anesthetic or muscle-relaxant drugs in the previous 24 hours.

Forms: If not ordering electronically, complete, print, and send 1 of the following forms with the specimen:

General Request Form (T239)

Neurology Test Request Form-General (T732) (http://www.mayomedicallaboratories.com/it-mmfiles/neurology-request-form.pdf)

Specimen Minimum Volume

2 mL

Specimen Stability Information

Specimen Type Temperature Time
Serum Refrigerated (preferred) 28 days
  Frozen  28 days
  Ambient  72 hours

Clinical Information

Myasthenia gravis (MG) is an acquired disorder of neuromuscular transmission caused by the binding of pathogenic autoantibodies to muscle's postsynaptic nicotinic acetylcholine receptor (AChR). Synaptic transmission fails when these pathogenic autoantibodies cause a critical loss of the AChR cation channel protein, which is required to activate the muscle action potential.

 

It is estimated that approximately 20% of adult patients have a paraneoplastic basis for MG. Thymoma is the most common neoplasm, often occult at the onset of MG, its diagnosis may precede MG onset. Thymoma is thought to be an endogenous source of muscle and neuronal antigens that drive production of characteristic autoantibodies. Other autoimmune neurological disorders sometimes accompany thymoma, with and without MG, including neuromuscular hyperexcitability, autonomic neuropathy, especially gastrointestinal dysmotilities encephalopathy, subacute hearing loss, or polymyositis.

 

MG can affect children as well as adults, but a paraneoplastic context is rare in children (neuroblastoma or thymoma are sometimes found).

 

Some of the antibodies in this profile are not pathogenic (eg, antibodies directed at cytoplasmic epitopes accessible in solubilized ion channels, or sarcomeric proteins that constitute the striational antigens).

 

Autoimmune serology is indispensable for initial evaluation and monitoring the course of patients with acquired MG. The neurological diagnosis depends on the clinical context, electromyographic findings, and response to anticholinesterase administration. MG is confirmed more readily by the individual patient's serological profile than by any single test.

 

See Myasthenia Gravis: Thymoma Diagnostic Algorithm in Special Instructions.

Reference Values

ACh RECEPTOR (MUSCLE) BINDING ANTIBODY

≤0.02 nmol/L

 

ACh RECEPTOR (MUSCLE) MODULATING ANTIBODIES

0-20% (reported as __% loss of AChR)

 

STRIATIONAL (STRIATED MUSCLE) ANTIBODIES

<1:120

 

CRMP-5-IgG WESTERN BLOT

Negative

 

AChR GANGLIONIC NEURONAL ANTIBODY

≤0.02 nmol/L

 

NEURONAL (V-G) K+ CHANNEL AUTOANTIBODY

≤0.02 nmol/L

 

GAD65 ANTIBODY ASSAY

≤0.02 nmol/L

Cautions

Because the autoantibody profile may change with tumor recurrence, single autoantibody testing is not recommended for follow-up after thymoma treatment.

 

A positive result in the myasthenia gravis (MG)/thymoma evaluation is not per se diagnostic of MG. Positive values for muscle acetylcholine receptor (AChR) and striational antibodies occur in 59% of patients with neurologically uncomplicated thymoma, 13% of Lambert-Eaton syndrome (LES) patients (Note: P/Q-type calcium channel antibodies are not found in MG, except for rare non-thymomatous paraneoplastic cases), 40% of patients with autoimmune liver disorders, approximately 10% of patients with lung cancer, and in patients with graft-versus-host disease, and recipients of D-penicillamine.

 

In this laboratory, false-positive results for AChR binding antibodies are excluded by reflexively retesting all positive sera with (125)I-alpha-bungarotoxin in the absence of muscle AChR. False-positive results occur most frequently in the bioassay for AChR modulating antibody; serum redraw will be requested when only this assay yields a positive result.

 

This test should not be requested in patients who have recently received radioisotopes, therapeutically or diagnostically, because of potential assay interference. The specific waiting period before specimen collection will depend on the isotope administered, the dose given and the clearance rate in the individual patient. Specimens will be screened for radioactivity prior to analysis. Radioactive specimens received in the laboratory will be held one week and assayed if sufficiently decayed, or canceled if radioactivity remains.

Day(s) Performed

ACh receptor (muscle) binding antibody: Monday through Friday 11:00 a.m., 6:00 p.m., and 10:00 p.m.; Saturday 6:00 a.m.; Sunday 6:00 a.m. and 10:00 a.m.

ACh receptor (muscle) modulating antibodies: Monday through Thursday; 2:00 p.m., Saturday; 8:00 a.m.

Striational (striated muscle) antibodies: Monday through Friday; 4:00 a.m. and 3:00 p.m.; Saturday 6:00 a.m.

CRMP-5-IgG Western blot: Monday, Wednesday, Friday; 8 a.m.

AChR ganglionic neuronal antibody: Monday through Friday 11:00 a.m. and 6:00 p.m.; Saturday 6:00 a.m.; Sunday 6:00 a.m.

Neuronal (V-G) K+ channel autoantibody: Monday through Friday 11:00 a.m. and 6:00 p.m.; Saturday 6:00 a.m.; Sunday 6:00 a.m.

GAD65 antibody assay: Monday to Friday; 6:00 a.m. and 4:00 p.m.

Report Available

3 days

Performing Laboratory

Mayo Medical Laboratories in Rochester

NY State Approved

Unknown