TY - JOUR
T1 - Newborn screening for cerebrotendinous xanthomatosis is the solution for early identification and treatment
AU - DeBarber, Andrea E.
AU - Kalfon, Limor
AU - Fedida, Ayalla
AU - Sheffer, Vered Fleisher
AU - Haroush, Shani Ben
AU - Chasnyk, Natalia
AU - Biton, Efrat Shuster
AU - Mandel, Hanna
AU - Jeffries, Krystal
AU - Shinwell, Eric S.
AU - Falik-Zaccai, Tzipora C.
N1 - Publisher Copyright:
Copyright © 2018 DeBarber et al. Published under exclusive license by The American Society for Biochemistry and Molecular Biology, Inc.
PY - 2018/11
Y1 - 2018/11
N2 - Cerebrotendinous xanthomatosis (CTX) is a progressive metabolic leukodystrophy. Early identification and treatment from birth onward effectively provides a functional cure, but diagnosis is often delayed. We conducted a pilot study using a two-tier test for CTX to screen archived newborn dried bloodspots (DBSs) or samples collected prospectively from a high-risk Israeli newborn population. All DBS samples were analyzed with flow injection analysis (FIA)-MS/ MS, and 5% of samples were analyzed with LC-MS/MS. Consecutively collected samples were analyzed to identify CTX-causing founder genetic variants common among Druze and Moroccan Jewish populations. First-tier analysis with FIA-MS/MS provided 100% sensitivity to detect CTX-positive newborn DBSs, with a low false-positive rate (0.1–0.5%). LC-MS/MS, as a second-tier test, provided 100% sensitivity to detect CTX-positive newborn DBSs with a false-positive rate of 0% (100% specificity). In addition, 5-cholestane-3,7,12,25-tetrol-3-O-D-glucuronide was identified as the predominant bile-alcohol disease marker present in CTX-positive newborn DBSs. In newborns identifying as Druze, a 1:30 carriership frequency was determined for the c.355delC CYP27A1 gene variant, providing an estimated disease prevalence of 1:3,600 in this population. These data support the feasibility of two-tier DBS screening for CTX in newborns and set the stage for large-scale prospective pilot studies.
AB - Cerebrotendinous xanthomatosis (CTX) is a progressive metabolic leukodystrophy. Early identification and treatment from birth onward effectively provides a functional cure, but diagnosis is often delayed. We conducted a pilot study using a two-tier test for CTX to screen archived newborn dried bloodspots (DBSs) or samples collected prospectively from a high-risk Israeli newborn population. All DBS samples were analyzed with flow injection analysis (FIA)-MS/ MS, and 5% of samples were analyzed with LC-MS/MS. Consecutively collected samples were analyzed to identify CTX-causing founder genetic variants common among Druze and Moroccan Jewish populations. First-tier analysis with FIA-MS/MS provided 100% sensitivity to detect CTX-positive newborn DBSs, with a low false-positive rate (0.1–0.5%). LC-MS/MS, as a second-tier test, provided 100% sensitivity to detect CTX-positive newborn DBSs with a false-positive rate of 0% (100% specificity). In addition, 5-cholestane-3,7,12,25-tetrol-3-O-D-glucuronide was identified as the predominant bile-alcohol disease marker present in CTX-positive newborn DBSs. In newborns identifying as Druze, a 1:30 carriership frequency was determined for the c.355delC CYP27A1 gene variant, providing an estimated disease prevalence of 1:3,600 in this population. These data support the feasibility of two-tier DBS screening for CTX in newborns and set the stage for large-scale prospective pilot studies.
KW - Bile acids and salts
KW - Diagnostic tools
KW - Inborn errors of metabolism
KW - Mass spectrometry
KW - Storage diseases
UR - http://www.scopus.com/inward/record.url?scp=85055907610&partnerID=8YFLogxK
U2 - 10.1194/jlr.M087999
DO - 10.1194/jlr.M087999
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C2 - 30135217
AN - SCOPUS:85055907610
SN - 0022-2275
VL - 59
SP - 2214
EP - 2222
JO - Journal of Lipid Research
JF - Journal of Lipid Research
IS - 11
ER -