Table 2:
List of genes associated with spliceosomopathies and ribosomopathies, their disease phenotypes, and known molecular function.
| Gene | Syndrome | Human Phenotype | References | Mutation | Function of Gene Product |
|---|---|---|---|---|---|
| SF3B4 | 1. Nager Syndrome 2. Rodriguez Syndrome |
Craniofacial – malar and mandibular hypoplasia, down-slanting palpebral fissures, external ear defects and cleft palate. Limb – primarily hypoplastic or absent thumbs. |
- Bernier et al., 2012 - Petit et al., 2013 - Champion-Arnaud and Reed, 2004 |
Frameshift or nonsense resulting in haploinsufficiency. | Member of SF3B complex of U2 snRNP involved in tethering U2 complex to branch site in pre-mRNA. |
| EFTUD2 | Mandibulofacial Dysostosis, Guion-Almeida Type (MFDGA) |
Craniofacial – overlaps with Nager syndrome and includes microcephaly. Limb – occasionally involves defects such as proximally placed thumbs and polydactyly of thumbs. |
- Lines et al., 2012 - Fabrizio et al., 1997 |
Frameshift, nonsense, missense, deletions resulting in haploinsufficiency. | Encodes the spliceosomal GTPase U5–116kD, a member of the U5 snRNP. |
| TXNL4A | Burn-Mckeow Syndrome |
Craniofacial – cleft lip and/or palate, short palpebral fissure, coloboma of the lower eyelids, prominent nasal bridge, and choanal atresia. Other – heart defects, large protruding ears. |
- Wieczorek et al., 2014 - Reuter et al., 1999 |
Heterozygous deletion in the promoter region of TXNL4A. | Yeast ortholog of TXNL4A (Dib1) encodes essential component of the U4/U6-U5 tri-snRNP complex |
| EIF4A3 | Richieri-Costa-Pereira Syndrome |
Craniofacial – midline cleft mandible, cleft palate, glossoptosis, and micrognathia. Limb – limb reductions and clubbed feet. |
- Favaro et al., 2014 - Andreou and Klostermeier 2013 |
Expansion of 18–20 nucleotide motifs in the 5’ UTR of EIF4A3. | Member of the exon junction complex (EJC). Anchors the EJC to the RNA. |
| SNRNPB | Cerebro-costo-mandibular Syndrome (CCMS) |
Craniofacial – cleft palate, glossoptosis, and micrognathia. Rib defects – posterior gaps and missing ribs. |
- Tooley et al., 2016 - Lynch et al., 2014 - Bacrot et al., 2014 - Will and Lührmann, 2011 |
SNRPB codes for three splice variants, one containing an alternative exon that contains a premature stop and functions to auto-regulate protein levels. In CCMS, mutation in the splicing silencer region of the alternative exon increase its inclusion and result in lower levels of SmB and SmB’. | SNRNPB-encoded SmB and SmB’ are splicing isoforms of one of the seven Sm proteins found in each snRNP. |
| CHD7 FAM172A | CHARGE Syndrome |
Coloboma of the eye, Heart defects, Atresia of choanae, Retardation of growth and development, Genital abnormalities, and Ear anomalies. Craniofacial – temporal bone anomalies and cleft lip and/or cleft palate. |
- Zentner et al., 2010 - Vissers et al., 2004 - Bajpai et al., 2010 - Schulz et al., 2014 |
Nonsense, missense, and single-copy 8q12 deletions of CHD7. | CHD7 is a chromatin remodeling factor that regulates the expression of key genes in the NCC GRN. |
| TCOF1, POLR1C, POLR1D, DDX2 | Treacher Collins Syndrome (TCS) |
Craniofacial – down-slanting palpebral fissures, micrognathia, facial bone hypoplasia, and cleft palate. Other – external ear defects, inner ear, and lower eyelid anomalies. |
- Fazen et al., 1967 - Phelps et al., 1981 - Edwards et al., 1997 - Dauwerse et al., 2011 - Valdez et al., 2004 - Gonzales et al., 2005 |
Mutations in the TCOF1 gene include splice site, missense, and nonsense mutations as well as insertions and deletions. | TCOF1, along with other factors, plays an important role in rDNA transcription and rRNA processing. |
| Ribosomal protein genes including: RPS19, RPS26, RPS27, RPL5, RPL11, GATA1 | Diamond-Blackfan anemia (DBA) |
Craniofacial – resemble defects observed in TCS. Limb – thumb abnormalities. Other – anemia caused by decrease of erythroid precursors. |
- Delaporta et al., 2014 - Kim et al., 2012 - Gazda et al., 2008 - Willing et al., 1999 - Fylgare et al., 2007 - Choesmel et al., 2007 - Doherty et al., 2010 - Sankaran et al., 2012 |
Mutations in RPS19 include nonsense, missense, frameshift, and splice site mutations as well as deletions. | RPS19 is required for 18S rRNA synthesis and 40S ribosomal subunit maturation. |