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VPS4A – de novo mutation (CIMDAG-Syndrome)[edit]
VPS4A-mutations (MIM:609982) cause a congenital ataxic multisystemic disorder with irregular neurodevelopment. This monogenetic de novo mutation can lead to structural brain abnormalities, severe neurodevelopmental delay, epilepsy, cataracts, growth impairment, and anemia.[1]
Signs and symptoms[edit]
The first sign of a VPS4A-mutation is a severe microcephaly (typically with Z scores <-5) followed by gross motor delays in early infancy, general neurodevelopmental delays with lack of developmental milestones (head control, turning, sitting, walking), intellectual disability, epileptic seizure onset, growth deficiency, and language impairment.[1][2] Severe intellectual or developmental disabilities are present in all known patients. All signs of infantile cerebral palsy like dystonia, dyskinesia, spasticity, ataxia, with profound neonatal onset of hypotonia can be observed. Persisting extrapyramidal symptoms with an ongoing plantar reflex (Babinsky sign) and Moro reflex. Integration disorder and sleep disorder (somnipathy) are also common. Patients may also suffer from significant feeding issues (needing a feeding tube) and constipation. Some patients experience nystagmus, strabismus, congenital cataracts, retinal dystrophy (Leber amaurosis), visual dysfunction or full blindness (nervus opticus atrophy).[1] Hearing seems to be less affected, although sensorineural deafness was observed.[1] Hip dysplasia, scoliosis and talipes are also common due to lack of mobility and spasticity. Some patients also develop hematologic problems, congenital dyserythropoietic anemia (CDA), hepatosplenomegaly or hepatosteatosis.[3]
Brain abnormalities[edit]
- cerebellar and/or vermal aplasia, hypoplasia and/or dysplasia[1]
- pontocerebral or cerebellar atrophy[1]
- bilateral polymicrogyria[1]
- thin and/or dysplastic corpus callosum[1]
- thickened calvarial vault
- brainstem hypoplasia[1]
- base of the skull can display abnormal signal hypointensity in relation with high proliferative hematopoiesis
- myelinization abnormalities or delay
VPS4A[edit]
The VPS4A-gene encodes the Vacuolar Protein Sorting-associated protein 4A ( VPS4A). This VPS4A protein belongs to the AAA-protein family (ATPases associated) with diverse cellular activities. VPS4A is involved in lysosomal/ endosomal membrane trafficking.[4] It also holds a key role in cytokinesis (midbody during abscission, concentrating at the spindle poles in the metaphase) and reticulocyte maturation through exosome biogenesis.[5] Cells lacking VPS4 (and/or its complex partner ESCRT-III) proteins develop aberrant nuclei, composed of fragmented or interconnected micronuclei, an increased number of centrosomes, multipolar spindles, and abnormal chromosome alignment during metaphase.[6]
Cause[edit]
The affected gene is located at the 16th Chromosome: 16q22.1; The actually known multiple heterozygous VPS4A loss-of-function mutations are present in general population databases. To the actual knowledge a haploinsufficiency mechanism is not considered to cause the type of severe early childhood condition.[1]
Missense variants[edit]
The VPS4A protein is a long molecule composed of a chain of 437 amino acids (aa). All genes have some amount of harmless variations in the general population, alike VPS4A, but in the middle of the VPS4A gene the background variation is reduced (~100aa-300aa). This area is relatively intolerant to genetic variation. Five of the probands published by Rodgers et al.[1] had de novo heterozygous missense variants at amino acid (aa) position 284 (four cases c.850A>T (p.Arg284Trp) substitution and one case with a c.850A>G (p.Arg284Gly)) change. One WES diagnosed a variant at c.616G>A (p.Glu206Lys).[1]
Not published is one case with a variant at position 284 c.605T>C Leu202Pro) in Germany, and one in England with a variant at position 116 (p.Ala116Thr). Further information is provided by the NCBI database.
Diagnosis[edit]
Diagnosis is based on genetic testing, with the recommended testing approach being whole exome sequencing (Trio-Exom-Analysis, WES and WGS).[1][7] EEG monitoring frequently shows generalized epilepsy. Seizure onset usually occurs within the 1st year of age. MRI points out the previously described brain abnormalities.
Seizure types[edit]
Seizure types most commonly follow the classification proposed by the International League Against Epilepsy (ILAE) in 1981.
- Atonic seizures
- Eyelid myoclonia
- Absence seizure
- Myoclonic jerks
- Tonic-clonic seizures
- Grand mal seizure
Treatment[edit]
There is currently no cure (e.g. gene therapy) or causative treatment. Epilepsy may be controlled by the use of one or more anti-epileptic drugs, vagus nerve stimulation,[8] or a ketogenic diet. At the actual state patients have seizures that are pharmacoresistant. Patients with significant feeding issues may require the use of a nasogastric, nasojejunal or gastric feeding tube. Communication may be supported with the use of an Augmentative and Alternative Communication device. Patients require the use of wheelchairs, adaptive strollers or Ankle Foot Orthoses. Supportive treatments can include:
- Occupational Therapy
- Physical Therapy
- Speech Therapy
- Equine-assisted Therapy
- Aquatic Therapy or Hydrotherapy
- Music Therapy
- Light Therapy
Prognosis[edit]
Two affected individuals died in childhood or early adult life. The oldest known patient is 30 years of age.[1]
Epidemiology[edit]
Actually 10 patients are known by the author of this article (6 published in the study by Rodgers et al.[1] 2020, 2 in England, 1 in Germany, 1 in Canada).[1]
Recommendations for parents[edit]
Facebook group: VPS4A mutation
The Undiagnosed Patients Program
CIMDAG -Syndrome[edit]
As proposed by Rodgers et al.[1] the “acronym CIMDAG (cerebellar hypoplasia and cataracts, intellectual disability, congenital microcephaly, dystonia and dyserythropoeitic anemia, growth retardation; MIM: 619273) may highlight the main clinical features of this syndrome, which may also include other structural brain abnormalities, retinal dystrophy, hepatosplenomegaly, and sensorineural deafness”.
Literature[edit]
- ^ a b c d e f g h i j k l m n o p Rodger, Catherine; Flex, Elisabetta; Allison, Rachel J.; Sanchis-Juan, Alba; Hasenahuer, Marcia A.; Cecchetti, Serena; French, Courtney E.; Edgar, James R.; Carpentieri, Giovanna; Ciolfi, Andrea; Pantaleoni, Francesca; Bruselles, Alessandro; Onesimo, Roberta; Zampino, Giuseppe; Marcon, Francesca (2020-12). "De Novo VPS4A Mutations Cause Multisystem Disease with Abnormal Neurodevelopment". The American Journal of Human Genetics. 107 (6): 1129–1148. doi:10.1016/j.ajhg.2020.10.012. PMC 7820634. PMID 33186545.
{{cite journal}}: Check date values in:|date=(help)CS1 maint: PMC format (link) - ^ Lunati, Ariane; Petit, Arnaud; Lapillonne, Hélène; Gameiro, Christine; Saillour, Virginie; Garel, Catherine; Doummar, Diane; Qebibo, Leila; Aissat, Abdelrazak; Fanen, Pascale; Bartolucci, Pablo; Galactéros, Fréderic; Funalot, Benoit; Burglen, Lydie; Mansour‐Hendili, Lamisse (2021-04). "VPS4A mutation in syndromic congenital hemolytic anemia without obvious signs of dyserythropoiesis". American Journal of Hematology. 96 (4). doi:10.1002/ajh.26099. ISSN 0361-8609.
{{cite journal}}: Check date values in:|date=(help) - ^ Seu, Katie G.; Trump, Lisa R.; Emberesh, Sana; Lorsbach, Robert B.; Johnson, Clarissa; Meznarich, Jessica; Underhill, Hunter R.; Chou, Stella T.; Sakthivel, Haripriya; Nassar, Nicolas N.; Seu, Kalani J.; Blanc, Lionel; Zhang, Wenying; Lutzko, Carolyn M.; Kalfa, Theodosia A. (2020-12). "VPS4A Mutations in Humans Cause Syndromic Congenital Dyserythropoietic Anemia due to Cytokinesis and Trafficking Defects". The American Journal of Human Genetics. 107 (6): 1149–1156. doi:10.1016/j.ajhg.2020.10.013. PMC 7820805. PMID 33186543.
{{cite journal}}: Check date values in:|date=(help)CS1 maint: PMC format (link) - ^ Maxfield, Frederick R.; McGraw, Timothy E. (2004-02-01). "Endocytic recycling". Nature Reviews Molecular Cell Biology. 5 (2): 121–132. doi:10.1038/nrm1315. ISSN 1471-0072.
- ^ Schöneberg, Johannes; Lee, Il-Hyung; Iwasa, Janet H.; Hurley, James H. (2017-01). "Reverse-topology membrane scission by the ESCRT proteins". Nature Reviews Molecular Cell Biology. 18 (1): 5–17. doi:10.1038/nrm.2016.121. ISSN 1471-0072. PMC 5198518. PMID 27703243.
{{cite journal}}: Check date values in:|date=(help)CS1 maint: PMC format (link) - ^ Morita, Eiji; Colf, Leremy A.; Karren, Mary Anne; Sandrin, Virginie; Rodesch, Christopher K.; Sundquist, Wesley I. (2010-07-20). "Human ESCRT-III and VPS4 proteins are required for centrosome and spindle maintenance". Proceedings of the National Academy of Sciences. 107 (29): 12889–12894. doi:10.1073/pnas.1005938107. ISSN 0027-8424. PMC 2919903. PMID 20616062.
{{cite journal}}: CS1 maint: PMC format (link) - ^ Turro, Ernest; Astle, William J.; Megy, Karyn; Gräf, Stefan; Greene, Daniel; Shamardina, Olga; Allen, Hana Lango; Sanchis-Juan, Alba; Frontini, Mattia; Thys, Chantal; Stephens, Jonathan; Mapeta, Rutendo; Burren, Oliver S.; Downes, Kate; Haimel, Matthias (2020-07-02). "Whole-genome sequencing of patients with rare diseases in a national health system". Nature. 583 (7814): 96–102. doi:10.1038/s41586-020-2434-2. ISSN 0028-0836. PMC 7610553. PMID 32581362.
{{cite journal}}: CS1 maint: PMC format (link) - ^ Kaniusas, Eugenijus; Kampusch, Stefan; Tittgemeyer, Marc; Panetsos, Fivos; Gines, Raquel Fernandez; Papa, Michele; Kiss, Attila; Podesser, Bruno; Cassara, Antonino Mario; Tanghe, Emmeric; Samoudi, Amine Mohammed; Tarnaud, Thomas; Joseph, Wout; Marozas, Vaidotas; Lukosevicius, Arunas (2019-08-09). "Current Directions in the Auricular Vagus Nerve Stimulation I – A Physiological Perspective". Frontiers in Neuroscience. 13: 854. doi:10.3389/fnins.2019.00854. ISSN 1662-453X. PMC 6697069. PMID 31447643.
{{cite journal}}: CS1 maint: PMC format (link) CS1 maint: unflagged free DOI (link)