CBS mutation screen

Description: 
Analysis of the CBS gene by PCR amplification and sequencing of the coding region and splice junctions is the gold standard approach.
Clinical details: 
Cystathionine b-Synthase deficiency is an autosomal recessive disorder resulting in homocystinuria - the most common inborn error of methionine metabolism. CBS deficiency results in elevated levels of homocysteine and methionine. The world-wide frequency is reported as ~1:300000 but is highly variable with frequencies as high as 1:65000 in Ireland and 1:20500 in Denmark and as low as 1:800000 in Japan. Causative mutations in the CBS gene are heterogeneous but there are recurrent mutations including the 'Celtic mutation' p.Gly307Ser, responsible for >70% of alleles in patients of celtic origin, and the pan-ethnic p.Ile278Thr, identified in nearly 25% of all CBS alleles.
Related condition or disease: 
CBS deficiency
Homocystinuria
Hyperhomocysteinemia
Reference range: 

n/a

Synonyms or keywords: 
CBS CBS deficiency Homocystinuria Hyperhomocysteinemia
Units: 
n/a
Department: 
Haemostasis and Thrombosis Department
Location: 
St Thomas' Hospital
Sample type and Volume required: 
1 x Edta
Call in advance: 
no
Turnaround time: 
8 weeks
Criteria for acceptance / rejections of sample
Storage and transport: 
transport at ambient temperature
Contacts:
Molecular Haemostasis Laboratory at St Thomas'
020 7188 2798
Haemostasis and Thrombosis
North Wing - 4th floor
St Thomas' Hospital
Westminster Bridge Road
London SE1 7EH

Laboratory opening times
Monday - Friday 09.00 - 17.00
For clinical advice or interpretation of results, please contact the laboratory in the first instance.
Laboratory: 
Molecular Haemostasis Laboratory at St Thomas'

Print as a PDF

Last updated: 14/03/2017