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PDE6B Related Disorders via the PDE6B Gene

Order Options and Pricing
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Summary and Pricing

Test Method

Exome Sequencing with CNV Detection
Test Code Test Copy GenesTest CPT Code Gene CPT Codes Copy CPT Codes Base Price
PDE6B 81479 81479,81479 $990
Test Code Test Copy Genes Test CPT Code Gene CPT Codes Copy CPT Code Base Price
11559PDE6B81479 81479,81479 $990 Order Options and Pricing

EMAIL CONTACTS

Genetic Counselors

Geneticist

  • Dana Talsness, PhD

Pricing Comments

Our favored testing approach is exome based NextGen sequencing with CNV analysis. This will allow cost effective reflexing to PGxome or other exome based tests. However, if full gene Sanger sequencing is desired for STAT turnaround time, insurance, or other reasons, please see link below for Test Code, pricing, and turnaround time information. If the Sanger option is selected, CNV detection may be ordered through Test #600.

An additional 25% charge will be applied to STAT orders. STAT orders are prioritized throughout the testing process.

Click here for costs to reflex to whole PGxome (if original test is on PGxome Sequencing platform).

Click here for costs to reflex to whole PGnome (if original test is on PGnome Sequencing platform).

The Sanger Sequencing method for this test is NY State approved.

For Sanger Sequencing click here.

Turnaround Time

3 weeks on average for standard orders or 2 weeks on average for STAT orders.

Please note: Once the testing process begins, an Estimated Report Date (ERD) range will be displayed in the portal. This is the most accurate prediction of when your report will be complete and may differ from the average TAT published on our website. About 85% of our tests will be reported within or before the ERD range. We will notify you of significant delays or holds which will impact the ERD. Learn more about turnaround times here.

Targeted Testing

For ordering sequencing of targeted known variants, go to our Targeted Variants page.

EMAIL CONTACTS

Genetic Counselors

Geneticist

  • Dana Talsness, PhD

Clinical Features and Genetics

Indications for Test

Patients with AR-RP and heterozygote carriers and patients with CSNBAD2 (OMIM 163500). This test may also be considered for the reproductive partners of individuals who carry pathogenic variants in PDE6B.

Clinical Features

Nonsyndromic retinitis pigmentosa (RP, OMIM # 268000) is a large group of inherited degenerative diseases of the retina characterized by abnormalities of the photoreceptors or the retinal pigment epithelium. It is a progressive disease. Symptoms usually begin with night blindness, progressing to constriction of the peripheral visual field with eventual loss of central vision. The age of onset varies from childhood to middle age (Gu et al. J Med Genet 36:705-707, 1999). The clinical hallmarks are an abnormal fundus with bone-spicule deposits and attenuated retinal vessels, abnormal electroretinographic findings, and reduced visual fields (Daiger et al. Arch Ophthalmol 125:151-158, 2007). RP affects 1 in 3,000 people worldwide (Farrar et al. EMBO J 21:857-864, 2002). Genetic abnormalities are the primary cause of RP, which affects all ethnic groups.

Genetics

Retinitis pigmentosa (RP) is genetically and clinically heterogeneous (Koenekoop Clin Experiment Ophthalmol 35:473-485, 2007). At least four distinct subgroups are recognized on the basis of the mode of inheritance: autosomal dominant (AD-RP), autosomal recessive (AR-RP), X-linked, and digenic (Kajiwara Science 264:1604-1608, 1994). In addition, RP can be inherited as a mitochondrial trait (Mansergh Am J Hum Genet 64:971-985, 1999). Genetic heterogeneity is documented within each subgroup. Currently, 23 genes are known to cause AR-RP. These include the PDE6B gene (McLaughlin et al. Nat Genet 4:130-134, 1993). At least 23 different PDE6B variants have been implicated in AR-RP. Although the majority of variants were missense and nonsense, splicing and small insertions or deletions were also reported. One homozygous gross insertion was found in affected individuals from a consanguineous Spanish family (Bayés et al. Hum Mutat 5:228-234, 1995). In addition to AR-RP, a heterozygous missense variant, His258Asp, was found in several affected individuals from a Dutch family with a strong history of congenital autosomal dominant stationary night blindness (CSNBAD2) (Gal et al. Nat Genet 7:551, 1994).The PDE6B gene encodes the beta subunit of rod phosphodiesterase, a key enzyme in phototransduction. 

Clinical Sensitivity - Sequencing with CNV PGxome

Variants in the PDE6B gene account for ~4% of patients with AR-RP (McLaughlin et al. Proc Natl Acad Sci USA 92:3249-3253, 1995).

Testing Strategy

This test provides full coverage of all coding exons of the PDE6B gene plus 10 bases of flanking noncoding DNA in all available transcripts along with other non-coding regions in which pathogenic variants have been identified at PreventionGenetics or reported elsewhere. We define full coverage as >20X NGS reads or Sanger sequencing. PGnome panels typically provide slightly increased coverage over the PGxome equivalent. PGnome sequencing panels have the added benefit of additional analysis and reporting of deep intronic regions (where applicable).

Dependent on the sequencing backbone selected for this testing, discounted reflex testing to any other similar backbone-based test is available (i.e., PGxome panel to whole PGxome; PGnome panel to whole PGnome).

Indications for Test

Patients with AR-RP and heterozygote carriers and patients with CSNBAD2 (OMIM 163500). This test may also be considered for the reproductive partners of individuals who carry pathogenic variants in PDE6B.

Gene

Official Gene Symbol OMIM ID
PDE6B 180072
Inheritance Abbreviation
Autosomal Dominant AD
Autosomal Recessive AR
X-Linked XL
Mitochondrial MT

Diseases

Name Inheritance OMIM ID
Night Blindness, Congenital Stationary, Rambusch Type AD 163500
Retinitis Pigmentosa 40 AR 613801

Citations

  • Bayes, M., et.al. (1995). "Homozygous tandem duplication within the gene encoding the beta-subunit of rod phosphodiesterase as a cause for autosomal recessive retinitis pigmentosa." Hum Mutat 5(3): 228-34. PubMed ID: 7599633
  • Daiger et al. 2007. PubMed ID: 17296890
  • Farrar, G. J., et.al. (2002). "On the genetics of retinitis pigmentosa and on mutation-independent approaches to therapeutic intervention." Embo J 21(5): 857-64. PubMed ID: 11867514
  • Gal, A., et.al. (1994). "Heterozygous missense mutation in the rod cGMP phosphodiesterase beta-subunit gene in autosomal dominant stationary night blindness." Nat Genet 7(4): 551. PubMed ID: 7951329
  • Gu S. et al. 1999. Journal of Medical Genetics. 36: 705-7. PubMed ID: 10507729
  • Kajiwara, K. et.al. (1994). "Digenic retinitis pigmentosa due to mutations at the unlinked peripherin/RDS and ROM1 loci." Science 264(5165): 1604-1608. PubMed ID: 8202715
  • Koenekoop, R. K., et.al. (2007). "Genetic testing for retinal dystrophies and dysfunctions: benefits, dilemmas and solutions." Clin Experiment Ophthalmol 35(5): 473-85. PubMed ID: 17651254
  • Mansergh, F. C., et.al. (1999). "Retinitis pigmentosa and progressive sensorineural hearing loss caused by a C12258A mutation in the mitochondrial MTTS2 gene." Am J Hum Genet 64(4): 971-85. PubMed ID: 10090882
  • McLaughlin, M. E., et.al. (1993). "Recessive mutations in the gene encoding the beta-subunit of rod phosphodiesterase in patients with retinitis pigmentosa." Nat Genet 4(2): 130-4. PubMed ID: 8394174
  • McLaughlin, M. E., et.al. (1995). "Mutation spectrum of the gene encoding the beta subunit of rod phosphodiesterase among patients with autosomal recessive retinitis pigmentosa." Proc Natl Acad Sci U S A 92(8): 3249-53. PubMed ID: 7724547

Ordering/Specimens

Ordering Options

We offer several options when ordering sequencing tests. For more information on these options, see our Ordering Instructions page. To view available options, click on the Order Options button within the test description.

myPrevent - Online Ordering

  • The test can be added to your online orders in the Summary and Pricing section.
  • Once the test has been added log in to myPrevent to fill out an online requisition form.
  • PGnome sequencing panels can be ordered via the myPrevent portal only at this time.

Requisition Form

  • A completed requisition form must accompany all specimens.
  • Billing information along with specimen and shipping instructions are within the requisition form.
  • All testing must be ordered by a qualified healthcare provider.

For Requisition Forms, visit our Forms page

If ordering a Duo or Trio test, the proband and all comparator samples are required to initiate testing. If we do not receive all required samples for the test ordered within 21 days, we will convert the order to the most effective testing strategy with the samples available. Prior authorization and/or billing in place may be impacted by a change in test code.

Specimen Types

Specimen Requirements and Shipping Details

PGxome (Exome) Sequencing Panel

PGnome (Genome) Sequencing Panel

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ORDER OPTIONS

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Note: acceptable specimen types are whole blood and DNA from whole blood only.
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