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IllnessHT amedes STANDARD heterozygosity test without sensorics genes

Summary

Short information

Applying this panel for central Europeans and other ethnicities asymptomatic individuals and couples are tested for being hetero- or hemizygous carriers for certain inherited disorders, excluding disturbed sensory, sexual differentiation and intellectual deficits.

ID
RP1092
Number of genes
102 Accredited laboratory test
Examined sequence length
288,3 kb (Core-/Core-canditate-Genes)
- (Extended panel: incl. additional genes)
Analysis Duration
on request
Test material
  • EDTA-anticoagulated blood (3-5 ml)
Diagnostic indications

NGS + X

 

Gene panel

Selected genes

NameExon Length (bp)OMIM-GReferenz-Seq.Heredity
ABCA35115NM_001089.3AR
ABCC84746NM_000352.6AD, AR
ABCD12238NM_000033.4XL
ACADM1266NM_000016.6AR
ACADVL1968NM_000018.4AR
ACAT11284NM_000019.4AR
AFF23936NM_002025.4XLR
AGA1041NM_000027.4AR
AGXT1179NM_000030.3AR
AHI13591NM_017651.5AR
AIRE1638NM_000383.4AD, AR
ALDOB1095NM_000035.4AR
ALPL1575NM_000478.6AD, AR
ANO101983NM_018075.5AR
ARSA1530NM_000487.6AR
ASL1395NM_000048.4AR
ASPA942NM_000049.4AR
ATP7B4398NM_000053.4AR
BBS11782NM_024649.5AR, digenisch
BBS22166NM_031885.5AR
BCKDHB1179NM_000056.5AR
BLM4254NM_000057.4AR
BTD1572NM_001370658.1AR
CBS1656NM_000071.3AR
CC2D2A4863NM_001080522.2AR
CCDC88C6087NM_001080414.4AD, AR
CEP2907440NM_025114.4AR
CFTR4443NM_000492.4AR
CHRNE1482NM_000080.4AD, AR
CLCN12967NM_000083.3AD, AR
COL7A18835NM_000094.4AD, AR
CPT21977NM_000098.3AD, AR
CYP11A11566NM_000781.3AR, AD
CYP21A21488NM_000500.9AR
CYP27A11596NM_000784.4AR
CYP27B11527NM_000785.4AR
DHCR71428NM_001360.3AR
DHDDS900NM_001243564.2AD, AR
DLD1530NM_000108.5AR
DMD11058NM_004006.3XLR
DYNC2H112945NM_001080463.2AR, digenisch
ELP13999NM_003640.5AR, AD
ERCC22283NM_000400.4AR
EVC23927NM_147127.5AD, AR
F87056NM_000132.4XLR
F91386NM_000133.4XL
FAH1260NM_000137.4AR
FANCC1677NM_000136.3AR
FKRP1488NM_024301.5AR
FKTN1386NM_001079802.2AR
FMO31599NM_001002294.3AR
GAA2859NM_000152.5AR
GALT1140NM_000155.4AR
GBA11611NM_001005741.3AD, AR
GBE12109NM_000158.4AR
GLA1290NM_000169.3XL
GNPTAB3771NM_024312.5AR
GRIP13231NM_021150.4AR
HBA1429NM_000558.5AD, AR
HBA2429NM_000517.6AD, AR
HBB444NM_000518.5AD, AR
HEXA1590NM_000520.6AR
HPS12103NM_000195.5AR
HPS33015NM_032383.5AR
IDUA1962NM_000203.5AR
L1CAM3774NM_000425.5XLR
LRP213968NM_004525.3AR
MCCC21692NM_022132.5AR
MCOLN11743NM_020533.3AR
MCPH12508NM_024596.5AR
MID12004NM_000381.4XLR
MLC11134NM_015166.4AR
MMACHC849NM_015506.3AR
MMUT2253NM_000255.4AR
MVK1191NM_000431.4AD, AR
NAGA1236NM_000262.3AR
NPHS13726NM_004646.4AR
NR0B11413NM_000475.5XL
OTC1065NM_000531.6XLR, XL
PAH1359NM_000277.3AR
PKHD112225NM_138694.4AR
PLP1834NM_000533.5XLR
PMM2741NM_000303.3AR
POLG3720NM_002693.3AR, AD
PRF11668NM_001083116.3AR
RARS21737NM_020320.5AR
RNASEH2B939NM_024570.4AR
RS1675NM_000330.4XL, XLR
SCO2801NM_005138.3AR
SLC19A31491NM_025243.4AR
SLC26A22220NM_000112.4AR
SLC26A42343NM_000441.2AR
SLC37A41291NM_001164277.2AR, AD
SLC6A81908NM_005629.4XLR
SMN1885NM_000344.4AR
SMPD11896NM_000543.5AR
TF2097NM_001063.4AR
TMEM216438NM_001173990.3AR
TNXB12729NM_019105.8AR, AD
TYR1590NM_000372.5AD, AR
USH2A15609NM_206933.4AR
XPC2823NM_004628.5AR

Informations about the disease

Clinical Comment

Based on professional recommendations (1), amedes offers a NGS panel to detect gene mutations associated with autosomal recessive and X-linked diseases. It includes 107 genes and their associated inherited diseases. The cut-off value for inclusion is a heterozygote frequency of ≥1:200 for autosomal recessive diseases (based on at least one U.S. subpopulation (2)).

The cumulative carrier frequency for pairs at risk (the probability that a pair studied has a heterozygous variant in at least one gene) depends strongly on the ethnicity and the degree of the relatedness (2).

References:

(1) Gregg et al; https://doi.org/10.1038/s41436-021-01203-z

(2) Schmidtke J, Krawczak M.; http://doi.org/10.1016/j.gim.2022.01.003

 

Synonyms
  • Alias: EHT amedes...
  • HT ersetzt EHT
  • Mutation carrier test; Carrier test
  • Für konsanguine Paare aus mitteleuropäischen und anderen Bevölkerungen ...
  • ...ohne Störungen der Sensorik, Geschlechtsdifferenzierung oder geistige Entwicklung
  • 3-methylcrotonyl CoA carboxylase 2 deficiency (MCCC2)
  • AR polycystic kidney disease (PKHD1)
  • Achondrogenesis Ib (SLC26A2)
  • Achromatopsia 3 (CNGB3)
  • Adrenal hypoplasia, congenital (NR0B1)
  • Adrenal insufficiency, congenital, with 46XY sex reversal, partial or complete (CYP11A1)
  • Adrenoleukodystrophy (ABCD1)
  • Aicardi Goutieres syndrome 2 (RNASEH2B)
  • Argininosuccinate aciduria (ASL)
  • Aspartylglucosaminuria (AGA)
  • Atransferrinemia (TF)
  • Autoimmune polyendocrinopathy syndrome type I (AIRE)
  • Bardet–Biedl syndrome 1 (BBS1)
  • Bardet–Biedl syndrome 2 (BBS2)
  • Basal ganglia disease, biotin-responsive (SLC19A3)
  • Biotinidase deficiency (BTD)
  • Bloom syndrome (BLM)
  • Canavan disease (ASPA)
  • Carbohydrate-deficient glycoprotein syndrome type Ia (PMM2)
  • Cardiomyopathy, dilated, 1X (FKTN)
  • Carnitine palmitoyltransferase II deficiency, infantile (CPT2)
  • Carnitine palmitoyltransferase II deficiency, lethal neonatal (CPT2)
  • Cerebral creatine deficiency syndrome 1 (SLC6A8)
  • Cerebrooculofacioskeletal syndrome 2 (ERCC2)
  • Cerebrotendinous xanthomatosis (CYP27A1)
  • Chondroectodermal dysplasia (EVC2)
  • Congenital adrenal hyperplasia due to 21-hydroxylase deficiency (CYP21A2)
  • Congenital disorder of glycosylation type 1 (DHDDS)
  • Congenital hydrocephalus 1 (CCDC88C)
  • Congenital myotonia, AR form (CLCN1)
  • Cystic fibrosis (CFTR)
  • Deafness AR 4 (SLC26A4)
  • Deafness, AR 23 (PCDH15)
  • Developmental and epileptic encephalopathy 1 (ARX)
  • Diabetes mellitus, permanent neonatal 3 (ABCC8)
  • Dihydrolipoamide dehydrogenase deficiency (DLD)
  • Donnai–Barrow syndrome (LRP2)
  • Ehlers–Danlos-like syndrome due to tenascin-X deficiency (TNXB)
  • Epiphyseal dysplasia, multiple, 4 (SLC26A2)
  • Fabry disease (GLA)
  • Familial dysautonomia (ELP1)
  • Fanconi anemia, complementation group C (FANCC)
  • Finnish congenital nephrotic syndrome (NPHS1)
  • Fragile X syndrome (FMR1)
  • Fraser syndrome (GRIP1)
  • Friedreich ataxia (FXN)
  • GBE1-related disorders (GBE)
  • Galactosemia (GALT)
  • Gaucher disease, type I (GBA)
  • Gaucher disease, type II (GBA)
  • Glycogen storage disease Ib (SLC37A4)
  • Glycogen storage disease Ic (SLC37A4)
  • Glycogen storage disease type IA (G6PC1)
  • Glycogen storage disease, type II, Pompe disease (GAA)
  • Glycogen storage disease, type IV (GBE)
  • Hemophagocytic lymphohistiocytosis, familial, 2 (PRF1)
  • Hemophilia A (F8)
  • Hemophilia B (F9)
  • Hereditary fructosuria (ALDOB)
  • Hermansky Pudlak syndrome 1 (HPS1)
  • Hermansky Pudlak syndrome 3 (HPS3)
  • Homocystinuria, B6 responsive + nonresponsive (CBS)
  • Hydrocephalus due to congenital stenosis of aqueduct of Sylvius (L1CAM)
  • Hyper-IgD syndrome (MVK)
  • Hyperoxaluria, primary type I (AGXT)
  • Hypophosphatasia, adult (ALPL)
  • Hypophosphatasia, childhood + infantile (ALPL)
  • Joubert syndrome 2 (TMEM216)
  • Joubert syndrome 3 (AHI1)
  • Joubert syndrome 5 (CEP290)
  • Joubert syndrome 9 (CC2D2A)
  • Leber congenital amaurosis 10 (CEP290)
  • Macular degeneration, XL atrophic (RPGR)
  • Maple syrup urine disease (BCKDHB)
  • Meckel syndrome 2 (TMEM216)
  • Meckel syndrome 6 (CC2D2A)
  • Medium-chain acyl-coenzyme A dehydrogenase deficiency (ACADM)
  • Megalencephalic leukoencephalopathy with subcortical cysts (MLC1)
  • Mental retardation, XL, associated with fragile site FRAXE (AFF2)
  • Metachromatic leukodystrophy (ARSA)
  • Methylmalonic aciduria with homocystinuria cblC type (MMACHC)
  • Methylmalonic aciduria–methylmalonyl–CoA mutase deficiency (MMUT)
  • Mevalonic aciduria (MVK)
  • Mitochondrial DNA depletion syndrome 4A (POLG)
  • Mitochondrial DNA depletion syndrome 4B (POLG)
  • Mitochondrial complex IV deficiency, nuclear type 2 (SCO2)
  • Mucolipidosis type II alpha/beta (GNPTAB)
  • Mucolipidosis type III alpha/beta (GNPTAB)
  • Mucolipidosis type IV (MCOLN1)
  • Mucopolysaccharidosis, Ich, Hurler S (IDUA)
  • Mucopolysaccharidosis, Ih/s, Hurler–Scheie S (IDUA)
  • Muscular dystrophy, Becker type (DMD)
  • Muscular dystrophy, Duchenne type (DMD)
  • Muscular dystrophy–dystroglycanopathy, type A, 5 (FKRP)
  • Muscular dystrophy–dystroglycanopathy, type B, 5 (FKRP)
  • Myasthenic syndrome, congenital, 4A, slow-channel (CHRNE)
  • Myasthenic syndrome, congenital, 4B, fast-channel (CHRNE)
  • Nemaline myopathy 2 (NEB)
  • Niemann–Pick disease, type A (SMPD1)
  • Niemann–Pick disease, type B (SMPD1)
  • Nonsyndromic hearing loss AD 3A (GJB2)
  • Nonsyndromic hearing loss AR 1A (GJB2)
  • Oculocutaneous albinism brown + type II (OCA2)
  • Oculocutaneous albinism type 1A + 1B (TYR)
  • Opitz GBBB syndrome, type I (MID1)
  • Ornithine transcarbamylase deficiency (OTC)
  • Pendred syndrome (SLC26A4)
  • Phenylketonuria (PAH)
  • Pontocerebellar hypoplasia type 6 (RARS2)
  • Primary microcephaly 1, AR (MCPH1)
  • Recessive dystrophic epidermolysis bullosa (COL7A1)
  • Retinitis pigmentosa 3 (RPGR)
  • Retinitis pigmentosa 59 (DHDDS)
  • Retinitis pigmentosa 74 (BBS2)
  • Retinitis pigmentosa, XL, + sinorespiratory infections, with/-out deafness (RPGR)
  • Retinoschisis 1, XL, juvenile (RS1)
  • Schindler disease, type 1 (NAGA)
  • Schindler disease, type 3 (NAGA)
  • Short-rib thoracic dysplasia 3 with or without polydactyly (DYNC2H1)
  • Sickle cell anemia β-thalassemia (HBB)
  • Smith–Lemli–Opitz syndrome (DHCR7)
  • Spastic paraplegia 2, XL (PLP1)
  • Spinal muscular atrophy types I, II, III, IV (SMN1)
  • Spinocerebellar ataxia 10 (ANO10)
  • Surfactant metabolism dysfunction, pulmonary 3 (ABCA3)
  • Tay–Sachs disease (HEXA)
  • Trichothiodystrophy 1, photosensitive (ERCC2)
  • Trimethylaminuria (FMO3)
  • Usher syndrome 3a (CLRN1)
  • Usher syndrome, type 1F (PCDH15)
  • Usher syndrome, type 2A (USH2A)
  • Very long chain acyl-CoA dehydrogenase deficiency (ACADVL)
  • Vitamin D–dependent rickets, type 1 (CYP27B1)
  • Walker–Warburg congenital muscular dystrophy (FKTN)
  • Wilson disease (ATP/B)
  • Xeroderma pigmentosum (XPC)
  • ɑ-Methylacetoacetic aciduria (ACAT1)
  • ɑ-Thalassemia (HBA1)
  • ɑ-Thalassemia (HBA2)
Heredity, heredity patterns etc.
  • AD
  • AR
  • XL
  • XLR
  • digenisch
OMIM-Ps
  • Multiple OMIM-Ps
ICD10 Code

Bioinformatics and clinical interpretation

No text defined