Test Catalog

Test ID: GID1    
Autoimmune Gastrointestinal Dysmotility Evaluation, Serum

Useful For Suggests clinical disorders or settings where the test may be helpful

Investigating unexplained weight loss, early satiety, anorexia, nausea, vomiting, constipation or diarrhea in a patient with past or family history of cancer or autoimmunity


Directing a focused search for cancer


Investigating gastrointestinal symptoms that appear in the course or wake of cancer therapy, not explainable by recurrent cancer, metastasis or therapy; detection of autoantibodies on this profile helps differentiate autoimmune gastrointestinal dysmotility from the effects of chemotherapy


Detecting early evidence of cancer recurrence in previously seropositive patients who have a rising titer of 1 or more autoantibodies

Testing Algorithm Delineates situations when tests are added to the initial order. This includes reflex and additional tests.

If IFA pattern is indeterminate, then WBN is performed at an additional charge.


If IFA pattern suggests CRMP-5-IgG, then CRMS and/or CRMWS are performed at an additional charge.


If IFA pattern suggests amphiphysin antibody, then AMPHS and/or ABLOT are performed at an additional charge.


If IFA pattern suggests antineuronal nuclear antibody, type 2; antineuronal nuclear antibody, type 3; Purkinje cell cytoplasmic antibody, type 1; Purkinje cell cytoplasmic antibody, type 2; Purkinje cell cytoplasmic antibody, type Tr; and/or anti-glial nuclear antibody, type 1; then ANN2S, ANN3S, PCABP, PCAB2, PCATR, and/or AGN1S are performed at an additional charge.


If IFA pattern suggests NMO/AQP4-IgG, then NMOFS is performed at an additional charge.


If NMO/AQP4-IgG FACS screen assay requires further evaluation, then NMO/AQP4-IgG FACS titration assay is performed at an additional charge.


If IFA pattern suggests NMDA-R, then NMDCS and/or NMDIS are performed at an additional charge.


If IFA pattern suggests AMPA-R, then AMPCS and/or AMPIS are performed at an additional charge.


If IFA pattern suggests GABA-B-R, then GABCS and/or GABIS are performed at an additional charge.


If acetylcholine (Ach) receptor binding antibody is >0.02, then ARMO and CRMWS are performed at an additional charge.


If VGKC >0.00, LGI1-IgG CBA, S and CASPR2-IgG CBA, S are performed at an additional charge.


See Autoimmune Gastrointestinal Dysmotility Evaluation Algorithm in Special Instructions.

Clinical Information Discusses physiology, pathophysiology, and general clinical aspects, as they relate to a laboratory test

Autoimmune gastrointestinal dysmotility (AGID) is a limited form of dysautonomia (also known as autoimmune autonomic ganglionopathy or neuropathy) that is sometimes a paraneoplastic disorder. Neoplasms most commonly found are lung cancer, thymoma, and miscellaneous adenocarcinomas. Diagnosis is confirmed by objective abnormalities on gastrointestinal (GI) motility studies (eg, gastric, small intestinal or colonic nuclear transit studies; esophageal, gastroduodenal, or colonic manometry or anorectal manometry with balloon expulsion). These disorders target autonomic postganglionic synaptic membranes and in some cases ganglionic neurons and autonomic nerve fibers, and may be accompanied by sensory small fiber neuropathy. Onset may be subacute or insidious. There may be additional manifestations of dysautonomia (eg, impaired pupillary light reflex, anhidrosis, orthostatic hypotension, sicca manifestations, and bladder dysfunction) or signs of other neurologic impairment. Autonomic reflex testing and a thermoregulatory sweat test are valuable aids in documentation of objective abnormalities.


The serological profile of AGID may include autoantibodies specific for onconeural proteins found in the nucleus, cytoplasm, or plasma membrane of neurons or muscle. Some of these autoantibodies are highly predictive of an underlying cancer. A commonly encountered autoantibody marker of AGID is the ganglionic neuronal alpha-3-AChR (acetylcholine receptor) autoantibody. The pathogenicity of this autoantibody was demonstrated in rabbits immunized with a recombinant extracellular fragment of the alpha-3-AChR subunit, and in mice injected with IgG from high-titered alpha-3-AChR autoantibody-positive rabbit or human sera. A direct relationship between antibody titer and severity of dysautonomia occurs in both experimental animals and patients. Patients with high alpha-3-AChR autoantibody values (>1.0 nmol/L) generally present with profound pandysautonomia, and those with lower alpha-3-AChR autoantibody values may have limited autoimmune dysautonomia, or other neurological symptoms and signs.


Importantly, cancer is detected in 30% of patients with alpha-3-AChR autoantibody. Cancer risk factors include the patient's past or family history of cancer, history of smoking, or social and environmental exposure to carcinogens. Early diagnosis and treatment of the neoplasm favors less morbidity from the GI dysmotility disorder. The cancers recognized most commonly with alpha-3-AChR autoantibody include adenocarcinomas of breast, lung, prostate, and GI tract, or lymphoma. A specific neoplasm is often predictable when a patient's autoantibody profile includes other autoantibodies to onconeural proteins shared by neurons, glia, or muscle. Small-cell lung carcinoma is found in 80% of antineuronal nuclear antibody-type 1 (ANNA-1) (anti-Hu)-positive patients and 23% of ANNA-1-positive patients have GI dysmotility. The most common GI manifestation is gastroparesis, but the most dramatic is pseudoobstruction.

Reference Values Describes reference intervals and additional information for interpretation of test results. May include intervals based on age and sex when appropriate. Intervals are Mayo-derived, unless otherwise designated. If an interpretive report is provided, the reference value field will state this.


Antineuronal Nuclear Ab, Type 1 (ANNA-1)


Antineuronal Nuclear Ab, Type 2 (ANNA-2)


Antineuronal Nuclear Ab, Type 3 (ANNA-3)


Anti-Glial/Neuronal Nuclear Ab, Type 1 (AGNA-1)




Purkinje Cell Cytoplasmic Ab, Type 1 (PCA-1)


Purkinje Cell Cytoplasmic Ab, Type 2 (PCA-2)


Purkinje Cell Cytoplasmic Ab, Type Tr (PCA-Tr)


Amphiphysin Antibody





Striational (Striated Muscle) Antibodies




Paraneoplastic Western Blot


CRMP-5-IgG Western Blot


Amphiphysin Western Blot




Glutamic Acid Decarboxylase (GAD65) Antibody

< or =0.02 nmol/L



N-Type Calcium Channel Antibody

< or =0.03 nmol/L

P/Q-Type Calcium Channel Antibody

< or =0.02 nmol/L

AChR Ganglionic Neuronal Antibody

< or =0.02 nmol/L

Neuronal VGKC Autoantibody

< or =0.02 nmol/L



ACh Receptor (Muscle) Binding Antibody

< or =0.02 nmol/L

AChR Receptor (Muscle) Modulating Antibody

0-20% loss of AChR


N-Methyl-D-aspartate receptor (NMDA-R)

CBA: Negative

IFA: <1:120

2-amino-3-(5-methyl-3-oxo-1,2-oxazol-4-yl) propanoic acid receptor (AMPA-R)

CBA: Negative

IFA: <1:120

Gamma-Amino Butyric acid-type B receptor (GABA-B-R)

CBA: Negative

IFA: <1:120

Leucine-Rich Glioma Inactivated Protein-1 IgG (LGI1)


Contactin-Associated Protein-Like-2 IgG (CASPR2)



Neuromyelitis Optica (NMO)/Aquaporin-4-IgG FACS Assay


Interpretation Provides information to assist in interpretation of the test results

Antibodies directed at onconeural proteins shared by neurons, muscle, and certain cancers are valuable serological markers of a patient's immune response to cancer. They are not found in healthy subjects, and are usually accompanied by subacute symptoms and signs. It is not uncommon for more than 1 antibody to be detected. Three classes of antibodies are recognized (the individual antibodies from each class included in the profile are denoted in parentheses):

-Antineuronal nuclear autoantibody-type 1

-Neuronal and muscle cytoplasmic (CRMP-5, glutamic acid decarboxylase, and striational)

-Plasma membrane cation channel (neuronal ganglionic [alpha-3-AChR (acetylcholine receptor)] and muscle AChR, neuronal voltage-gated N-type calcium channel, neuronal voltage-gated potassium channel antibodies). All of these autoantibodies are potential effectors of autoimmune gastrointestinal dysmotility.

Cautions Discusses conditions that may cause diagnostic confusion, including improper specimen collection and handling, inappropriate test selection, and interfering substances

Negative results do not exclude autoimmune gastrointestinal dysmotility or cancer.

Clinical Reference Recommendations for in-depth reading of a clinical nature

1. Lennon VA, Sas DF, Busk MF, et al: Enteric neuronal autoantibodies in pseudo-obstruction with small cell lung carcinoma. Gastroenterology 1991;100:137-142

2. Lucchinetti CF, Kimmel DW, Lennon VA: Paraneoplastic and oncological profiles of patients seropositive for type 1 anti-neuronal nuclear autoantibodies. Neurology 1998;50:652-657

3. Vernino S, Adamski J, Kryzer TJ, et al: Neuronal nicotinic ACh receptor antibody in subacute autonomic neuropathy and cancer-related syndromes. Neurology 1998;50:1806-1813

4. Vernino S, Low PA, Fealey RD, et al: Autoantibodies to ganglionic acetylcholine receptors in autoimmune autonomic neuropathies. N Engl J Med 2000;343:847-855

5. Dhamija R, Tan KM, Pittock SJ, et al: Serological profiles aiding the diagnosis of autoimmune gastrointestinal dysmotility. Clin Gastroenterol Hepatol 2008;6:988-992

6. McKeon A, Lennon VA, Lachance DH, et al: The ganglionic acetylcholine receptor autoantibody: oncological, neurological and serological accompaniments. Arch Neurol 2009;66(6):735-741

7. Kraichely RE, Farrugia G, Castell DO, et al: Neural autoantibody profile of primary achalasia. Dig Dis Sci 2010 Feb;55(2):307-311

Special Instructions Library of PDFs including pertinent information and forms related to the test