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FAQ: What is the turnaround time
for the Ambry Tests: Canavan AMPLIFIED & Tay-Sachs Plus?
Canavan AMPLIFIED results
are reported in 2-4 weeks.
Tay-Sachs plus results are reported in 3-5 weeks.
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Canavan and Tay-Sachs Diseases |
Canavan and Tay-Sachs Diseases are both severe
neurodegenerative disorders with increased carrier rates in
the Ashkenazi Jewish population. Molecular testing for a small
number of mutations is highly sensitive in that population,
but not in other ethnic groups. Full gene sequence analysis
at Ambry Genetics provides a detection rate of 99% across all
ethnicities. This enables the greatest possible carrier risk
reduction for high-risk or mixed-ethnicity couples, expands
options for prenatal diagnosis, simplifies carrier testing in
the extended family, and clarifies or confirms biochemical diagnoses.
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The Ambry Test®: Canavan AMPLIFIED™ |
Canavan Disease results from mutations in the
ASPA gene and disruption of myelination of the central nervous
system. Onset occurs in infancy with hypotonia, progressive
loss of motor control, and macrocephaly. Patients usually do
not survive past childhood. The most common mutations account
for only about 50% of those found in the non-Ashkenazi Jewish.
More than 50 disease-causing mutations, including gross deletions,
have been reported. Biochemical carrier testing is not available
for screening purposes.
The test is a full gene sequence analysis of ASPA. In addition,
gross deletion/duplication analysis of the entire ASPA gene
is performed to detect known and potential novel gross deletions.
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The Ambry Test: Tay-Sachs Plus |
Tay-Sachs Disease is a lysosomal storage disorder caused by
HEXA gene mutations. Most cases are rapidly progressive with
infantile onset. Late onset Tay-Sachs with childhood or early
adult presentation is caused by HEXA mutations that allow residual
Hex A enzyme activity. Enzyme analysis is a sensitive carrier
screening and diagnostic tool that should be used in all cases.
However, DNA analysis serves as a valuable complement when:
- Carrier screens have indeterminate results
- Approximately 36%
of enzymatically-defined non-Ashkenazi Jewish and 2% of Ashkenazi
Jewish “carriers” are actually pseudodeficiency
mutation carriers with no increased risk for affected children
- Disease variants and mutations in other
genes can cause symptoms and mask enzyme abnormalities
Ambry Genetics requires enzyme analysis prior
to Tay-Sachs Plus for carrier and diagnostic tests. Full gene
sequence analysis can detect the 100+ described HEXA mutations.
Together these tests provide the highest possible sensitivity
and specificity.
The test is a full gene sequence analysis of
HEXA. In addition, the 7.6 kb French-Canadian deletion and two
pseudodeficiency mutations are detected.
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Clinical Indications |
- Carrier testing for high-risk, anxious,
or mixed-ethnicity couples
- Prenatal diagnosis on CVS or amniotic fluid
for known carrier couples
- Mutation definition in affected patients
- Resolution of indeterminate or pseudodeficient
Tay-Sachs enzyme results
- Diagnostic clarification in patients with
Tay-Sachs symptoms and inconsistent enzyme results
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Revised Carrier Risks |
The following table shows revised or post-test
carrier risks by ethnicity, assuming a negative Ambry Test result
and no family history of the disease.
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Ethnicity
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Canavan
Carrier Risk Before Test
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Revised
Carrier Risk after Canavan AMPLIFIED
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Tay-Sachs
Carrier Risk Before Test
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Revised
Carrier Risk after Tay-Sachs Plus*
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| Ashkenazi
Jewish |
1/57 |
1/5601 |
1/30 |
1/2901 |
| Other
populations at general risk |
unknown;
<1/57 |
<1/5601 |
1/280 |
1/27,901 |
| Cajun,
French-Canadian
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unknown;
<1/57 |
<1/5601 |
1/30 |
1/2901 |
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Irish
American |
unknown;
<1/57 |
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1/44 |
1/4301 |
*Calculation excludes consideration
of enzyme analysis results.
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Canavan and Tay-Sachs Diseases Materials |
 The
Ambry Tests: Canavan AMPLIFIED & Tay-Sachs Plus
General Test Information
The
Ambry Test: Canavan AMPLIFIED
(Abobe PDF document)
General Test Information
The
Ambry Test: Tay-Sachs Plus
(Abobe PDF document)
The following CPT Codes for The Ambry Test
reflects Ambry Genetics’ interpretation of CPT coding
requirements based on AMA guidelines:
Ambry Test: Canavan AMPLIFIED
83891, 83894, 83898, 83900, 83901, 83904, 83909,
83912
Ambry Test: Tay-Sachs Plus
83891, 83894, 83898, 83904, 83909, 83912
CPT codes are provided only as a guide
to assist you in billing. CPT coding is the sole responsibility
of the billing party.
Disclaimer:
This test was developed and its performance characteristics
were determined by Ambry Genetics Corporation. The laboratory
is regulated under the Clinical Laboratory Improvement Amendments
2003 as qualified to perform nonwaived testing.
The Ambry Test: Canavan AMPLIFIED analyzes the following types
of mutations: nucleotide substitutions, small deletions, small
insertions, small indels, gross deletions, and gross duplications.
It is not intended to analyze the following types of mutations:
gross insertions, gene rearrangements, deep intronic variations,
and other unknown abnormalities. The pattern of mutation types
varies with the gene tested and the Ambry Test detects a high
but variable percentage of known and unknown mutants of the
classes stated. A negative result from the analysis cannot rule
out the possibility that the tested individual carries a rare
unexamined mutation or mutation in the undetectable group. The
Ambry Test: Canavan AMPLIFIED is designed and validated to be
capable of detecting about ~99% of Canavan Disease mutations,
respectively (considering less than 1% being the other types
of mutations). Canavan Disease is a complex clinical disorder,
which in the majority of cases is due to alterations in the
ASPA gene generally detected by The Ambry Test: Canavan AMPLIFIED
except as noted above. Mutations in other genes or the regions
not tested by The Ambry Test: Canavan AMPLIFIED can also give
rise to clinical conditions similar or identical to Canavan
Disease.
The Ambry Test: Tay-Sachs Plus analyzes the following types
of mutations: nucleotide substitutions, small deletions, small
insertions, and small indels and is not intended to analyze
the following types of mutations: gross deletions (except the
7.6kb French-Canadian deletion), gross duplications, gross insertions,
gene rearrangements, deep intronic variations, and other unknown
abnormalities. The pattern of mutation types varies with the
gene tested and the Ambry Test detects a high but variable percentage
of known and unknown mutants of the classes stated. A negative
result from the analysis cannot rule out the possibility that
the tested individual carries a rare unexamined mutation or
mutation in the undetectable group. The Ambry Test: Tay-Sachs
Plus is designed and validated to be capable of detecting about
~99% of Tay-Sachs Disease mutations (considering less than 1%
to be the other types of mutations). Tay-Sachs Disease is a
complex clinical disorder, which in the majority of cases is
due to alterations in the HEXA gene generally detected by The
Ambry Test: Tay-Sachs Plus except as noted above. Mutations
in other genes or the regions not tested by The Ambry Test:
Tay-Sachs Plus can also give rise to clinical conditions similar
or identical to Tay-Sachs Disease.
Although molecular tests are highly accurate, rare diagnostic
errors may occur. Possible diagnostic errors include sample
mix-up, erroneous paternity identification, technical errors,
and genotyping errors. Genotyping errors can result from trace
contamination of PCR reactions, from maternal cell contamination
in fetal samples, from rare genetic variants, which interfere
with analysis, or from other sources. This report does not represent
medical advice. Any questions, suggestions, or concerns regarding
interpretation of results should be forwarded to a genetic counselor,
medical geneticist, or physician skilled in interpretation of
the relevant medical literature. References are available upon
request.
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