4.6 Article

Second Tier Testing to Reduce the Number of Non-actionable Secondary Findings and False-Positive Referrals in Newborn Screening for Severe Combined Immunodeficiency

Journal

JOURNAL OF CLINICAL IMMUNOLOGY
Volume 41, Issue 8, Pages 1762-1773

Publisher

SPRINGER/PLENUM PUBLISHERS
DOI: 10.1007/s10875-021-01107-2

Keywords

TRECs; Newborn screening; Severe combined immunodeficiency; SCID; Inborn errors of immunity; Second tier; Epigenetic immune cell counting; Next-generation sequencing; NGS

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Funding

  1. Netherlands Organisation for Health Research and Development ZonMw [543002002]

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The use of a second PCR analysis method and different primers can reduce false-positive referrals in newborn screening for SCID. Adjusting the TREC cutoff value or screening algorithm can lower referral rates, but cannot prevent all false-positive referrals.
Purpose Newborn screening (NBS) for severe combined immunodeficiency (SCID) is based on the detection of T-cell receptor excision circles (TRECs). TRECs are a sensitive biomarker for T-cell lymphopenia, but not specific for SCID. This creates a palette of secondary findings associated with low T-cells that require follow-up and treatment or are non-actionable. The high rate of (non-actionable) secondary findings and false-positive referrals raises questions about the harm-benefit-ratio of SCID screening, as referrals are associated with high emotional impact and anxiety for parents. Methods An alternative quantitative TREC PCR with different primers was performed on NBS cards of referred newborns (N = 56) and epigenetic immune cell counting was used as for relative quantification of CD3 + T-cells (N = 59). Retrospective data was used to determine the reduction in referrals with a lower TREC cutoff value or an adjusted screening algorithm. Results When analyzed with a second PCR with different primers, 45% of the referrals (25/56) had TREC levels above cutoff, including four false-positive cases in which two SNPs were identified. With epigenetic qPCR, 41% (24/59) of the referrals were within the range of the relative CD3 + T-cell counts of the healthy controls. Lowering the TREC cutoff value or adjusting the screening algorithm led to lower referral rates but did not prevent all false-positive referrals. Conclusions Second tier tests and adjustments of cutoff values or screening algorithms all have the potential to reduce the number of non-actionable secondary findings in NBS for SCID, although second tier tests are more effective in preventing false-positive referrals.

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