Dyskeratosis Congenita (DC) via the NHP2 Gene

Dyskeratosis congenita (DC) is characterized by multiple anomalies including abnormal skin pigmentation, nail dystrophy, mucosal leukoplakia, bone marrow failure and an increase in cancer predisposition (Walne et al. 2007. PubMed ID: 17507419; Kirwan et al. 2008. PubMed ID: 18005359). Individuals affected with DC can exhibit other features including liver cirrhosis, osteoporosis, pulmonary fibrosis and learning difficulties. Approximately 80-90% individuals affected with DC experience bone marrow failure by age 30 (Kirwan et al. 2008. PubMed ID: 18005359). Age of onset and progression of DC may vary. Those who have minimal physical findings with normal bone marrow function are at the mild end of the spectrum, while those at the severe end of the spectrum have these features along with bone marrow failure (Savage et al. 2016. PubMed ID: 20301779).

Dyskeratosis congenita (DC) is caused primarily by defects in telomere maintenance (Walne et al. 2007. PubMed ID: 17507419; Trahan et al. 2010. PubMed ID: 20008900). DC is characterized by three genetic subtypes: X-linked recessive, caused by variants in the DKC1 gene, autosomal dominant DC caused by heterozygous variants in TERC, TINF2 or TERT genes, and autosomal recessive DC which involves several genes including ACD, CTC1, DKC1, NHP2, NOP10, PARN, RTEL1, WRAP53 and TERT (Savage et al. 2016. PubMed ID: 20301779). NHP2-related DC is inherited in an autosomal recessive manner, and variants in the NHP2 gene account for <1% of pathogenic variants reported in DC patients.

The NHP2 gene encodes nucleolar protein family A, member 2 (NOLA2), which is required for ribosomal biogenesis and telomere maintenance. To date, three pathogenic variants have been reported in the NHP2 gene (c.376G>A, p.V126M, c.415T>C, p.Y139H and c.460T>A, p.*154Argext*51) (Human Gene Mutation Database; Vulliamy et al. 2008. PubMed ID: 18523010; Trahan et al. 2010. PubMed ID: 20008900).

Approximately 70% of individuals with dyskeratosis congenita (DC) have pathogenic variants in at least 1 of the 11 known DC genes. Pathogenic variants in the NHP2 gene account for <1% of DC cases.

This test provides full coverage of all coding exons of the NHP2 gene plus 10 bases of flanking noncoding DNA in all available transcripts along with other non-coding regions in which pathogenic variants have been identified at PreventionGenetics or reported elsewhere. We define full coverage as >20X NGS reads or Sanger sequencing. PGnome panels typically provide slightly increased coverage over the PGxome equivalent. PGnome sequencing panels have the added benefit of additional analysis and reporting of deep intronic regions (where applicable).

Dependent on the sequencing backbone selected for this testing, discounted reflex testing to any other similar backbone-based test is available (i.e., PGxome panel to whole PGxome; PGnome panel to whole PGnome).