Newborn Screening and T-Cell Receptor Excision Circles

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Newborn Screening
 
Chase. Curr. Opin. All. Imm. 2010, 10:521–5256
 
Chase. Curr. Opin. All. Imm. 2010, 10:521–5256
 
 
Generation of a unique
T-cell receptor (TCR)
clone begins by random
selection and
combination of TCR
regions in germ line DNA
The excised DNA
sequences form a non-
replicating episome
TREC-positive cells are
recent thymic emigrants
 
T-Cell Receptor Excision Circles (TRECs)
 
Hazenberg. J. Mol. Med. 2001, 79:631–640
 
T-Cell Receptor Excision Circles (TRECs)
 
 
TRECs can be detected
in peripheral blood by
quantitative PCR
 
TREC levels correlate
with numbers of naïve T-
cells
Low TREC levels
associated with SCID,
diGeorge syndrome,
congenital lymphopenia
 
* Hale. J. All. Clin. Immunol. 2010, 126:1073–4
 
T-Cell Receptor Excision Circles (TRECs)
 
 
2008: Wisconsin became first state to include TREC
quantitation in the newborn screen
 
2009: The first infant with SCID identified in
Massachusetts*
 
2010: TREC assay added to New York newborn
screen
undefined
 
Chase. Curr. Opin. All. Imm. 2010, 10:521–5256
 
TREC Assay Pitfalls and Future Directions
 
 
Reference ranges have not been established for
neonates < 37 weeks corrected gestation
 
Many abnormal TREC results have lead to diagnosis of
undefined T-cell immunodeficiencies; without identifying
underlying genetic defect optimal management remains
uncertain
 
Multi-plex quantitative PCR methods are being
developed to screen for additional genetic diseases
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The content discusses the importance of newborn screening, characteristics of disorders, T-cell receptor excision circles (TRECs), and the identification of severe conditions like SCID through TREC assay. It highlights the significance of early detection and treatment, emphasizing the value of high-throughput screening methods and the potential future directions in TREC assays for genetic disease screening.

  • Newborn Screening
  • T-Cell Receptor
  • Early Detection
  • TRECs
  • Genetic Diseases

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  1. TREC SCREENING

  2. Newborn Screening Characteristics of Test Characteristics of Disorders Well characterized pathogenesis Affects a significant number of infants Undetectable by routine examination Result in devastating consequences if not diagnosed/treated early Disease-altering treatment available High sensitivity and specificity Amenable for high- throughput screening Favorable cost-benefit analysis Low risk to infant Means of providing follow up Chase. Curr. Opin. All. Imm. 2010, 10:521 5256

  3. T-Cell Receptor Excision Circles (TRECs) Generation of a unique T-cell receptor (TCR) clone begins by random selection and combination of TCR regions in germ line DNA The excised DNA sequences form a non- replicating episome TREC-positive cells are recent thymic emigrants Chase. Curr. Opin. All. Imm. 2010, 10:521 5256

  4. T-Cell Receptor Excision Circles (TRECs) TRECs can be detected in peripheral blood by quantitative PCR TREC levels correlate with numbers of na ve T- cells Low TREC levels associated with SCID, diGeorge syndrome, congenital lymphopenia Hazenberg. J. Mol. Med. 2001, 79:631 640

  5. T-Cell Receptor Excision Circles (TRECs) 2008: Wisconsin became first state to include TREC quantitation in the newborn screen 2009: The first infant with SCID identified in Massachusetts* 2010: TREC assay added to New York newborn screen * Hale. J. All. Clin. Immunol. 2010, 126:1073 4

  6. Chase. Curr. Opin. All. Imm. 2010, 10:5215256

  7. TREC Assay Pitfalls and Future Directions Reference ranges have not been established for neonates < 37 weeks corrected gestation Many abnormal TREC results have lead to diagnosis of undefined T-cell immunodeficiencies; without identifying underlying genetic defect optimal management remains uncertain Multi-plex quantitative PCR methods are being developed to screen for additional genetic diseases

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