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Laboratory Perspective of screening

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... HPLC/Electrophoresis ... Testing regimes for high and low prevalence areas Family Origin Questionnaire Outline of the investigation scheme for haemoglobin ... – PowerPoint PPT presentation

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Title: Laboratory Perspective of screening


1
Laboratory Perspective of screening
  • Joan Henthorn
  • Central Middlesex Hospital
  • London UK
  • July 2009

2
Screening versus Diagnosis
  • Screening systematic testing of a whole or
    selected population
  • Uses fast throughput technique
  • Often used to target certain conditions
  • Diagnosis the intensive investigation of a
    individual or family using many different
    techniques to arrive at a conclusion

All screening
3
AIMS OF SCREENING
  • NEONATAL
  • To detect individuals who will benefit from early
    diagnosis and treatment, thus reducing morbidity
    and mortality
  • Cascade family screening
  • To target at risk families and offer future
    genetic choice
  • To allow better Health Service resource planning
  • ANTENATAL
  • To target at risk couples and offer genetic
    choice
  • To offer family screening
  • To detect individuals with sickle cell syndromes
    who will benefit from diagnosis and treatment,
    thus reducing morbidity and mortality

Antenatal and neonatal
4
The aim of the programme is to detect the
following
  • NEONATAL
  • SS
  • SC
  • SD
  • SO-ARAB
  • SBETA
  • ANTENATAL
  • S
  • C
  • D-Punjab
  • E
  • O-Arab
  • Beta thal trait
  • Delta/beta thal trait
  • Alpha0 thal trait
  • Lepore

Antenatal and neonatal
5
Neonatal Screening Programme - England
  • Universal
  • Use dried blood spots
  • Contemporaneously with PKU and Thyroid
  • First line screen to be either HPLC or IEF
  • Second line confirmation to be either IEF or HPLC

Neonatal
6
What we cannot detect with Neonatal Screening
  • Beta thalassaemia trait
  • Some cases of beta thalassaemia intermedia
  • Some rare variants
  • HPFH

Neonatal
7
Antenatal Screening Programme - England
  • Areas are defined as high or low prevalence
  • High prevalence is defined as a foetal prevalence
    rate for sickle cell disease of 1.5 or more per
    10000 pregnancies

8
Testing regimes for high and low prevalence areas
  • High prevalence
  • All samples tested for thalassaemia and Hb
    variants by laboratory methods
  • Family origin question used to assess the need
    for partner testing in cases of possible alpha0
    thalassaemia
  • Low prevalence
  • All samples screened for thalassaemia using red
    cell indices
  • All women assessed for laboratory testing for
    variants by use of the family origin question
  • Family origin question used to assess the need
    for partner testing in cases of possible alpha0
    thalassaemia

9
Family Origin Questionnaire
10
Outline of the investigation scheme for
haemoglobin disorders
Antenatal
11
Outline of the investigation scheme for
haemoglobin disorders
Antenatal
12
Risk assessment of using the algorithm
  • Silent or near silent ?-thalassaemia trait
  • Possibly some ?-thalassaemias obscured by severe
    iron deficiency anaemia
  • ?0thalassaemia occurring outside the defined at
    risk groups
  • Dominant haemoglobinopathies in the partner when
    the woman is AA, - very rare and should be
    suggested by the family history
  • Some women may not be tested if the ethnic group
    is incorrectly stated or hidden.
  • ?-thalassaemia obscured by B12/folate deficiency
    or liver disease
  • Hb S, C, DPunjab, E, OArab in the North-European
    ethnic group

13
Challenges - General
  • What should we report?
  • How should we report it?
  • How should we report it if we dont know exactly
    what it is?
  • How should we convey what we cant detect?

All screening
14
Challenges - Neonatal
  • Transfused babies
  • Premature babies
  • Older babies/ Old samples
  • Gamma chain variants
  • Variants on HPLC and not IEF
  • Variants on IEF and not on HPLC
  • Conflicts between childs result and parental
    results

Neonatal
15
Challenges - Antenatal
  • A2 variants
  • Alpha/beta interactions
  • Silent beta thalassaemia trait
  • Alpha thalassaemia
  • B12/Folate/Iron deficiency
  • Borderline raised A2 values
  • HIV
  • Sporadic

Antenatal
16
What we aim to provide
  • Agreed turnaround times
  • Readable reports with explanations and
    recommended actions
  • Advice if needed

17
Report elements (Antenatal)
  • The numeric data
  • FBC (Hb,MCV and MCH)
  • The A2
  • Any Variants found
  • Interpretation of the results
  • The action recommended

18
What we expect to receive
  • Properly labelled samples and legible forms
  • Partners correctly identified

19
LINKAGE the final frontier
  • The antenatal and neonatal screening in England
    are intended to be linked programmes
  • For each baby, the antenatal results should be
    available at the time of the neonatal screen.
  • The neonatal result should be used to crosscheck
    that each couple had the appropriate antenatal
    screening offered and carried out.
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