NFIA Haploinsufficiency Is Associated with a CNS Malformation Syndrome and Urinary Tract Defects

Lu, Weining; Quintero‐Rivera, Fabiola; Fan, Yanli; Alkuraya, Fowzan S.; Donovan, Diana; Xi, Qiongchao; Turbé-Doan, Annick; Li, Qinggang; Campbell, Craig; Shanske, Alan; Sherr, Elliott H.; Ahmad, Ayesha; Peters, Roxana; Rilliet, Bénédict; Parvex, Paloma; Bassuk, Alexander G.; Harris, David J.; Ferguson, Heather; Kelly, Chantal; Walsh, Christopher A.; Gronostajski, Richard M.; Devriendt, Koenraad; Higgins, Anne W.; Ligon, Azra H.; Quade, Bradley J.; Morton, Cynthia C.; Gusella, James F.; Maas, Richard L.

doi:10.1371/journal.pgen.0030080

Cited by 111 publications

(133 citation statements)

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“…2,3 Mechanistically, Bortezomib binds the active sites of the enzymes in the b-subunits located in the proteolytic chamber of the 20S proteasome. 4 Molecules that inhibit the proteasome through a different mechanism would be useful probes to understand the activity of this enzyme complex and potentially new therapeutic agents.…”

Section: Acknowledgementsmentioning

confidence: 99%

“…1 The NFI proteins comprise a DNA binding and dimerization domain in their N-terminal half, which contains four cysteine residues common to the four vertebrate members and conserved in the nonvertebrate orthologs, and a transactivation and repression domain in their C-terminal half (Figure 1a). The NFIA gene, located in the 1p31 chromosomal region, has a function in brain, [2][3][4] ureteral and renal development 3 as well as hematopoiesis. 5,6 Interactions of NFIA with CEBPa and PU.1 through microRNAs regulate granulocytic and monocytic differentiation, respectively.…”

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confidence: 99%

“…However, NFIA haplo-insufficiency has a deleterious effect when occurring in germinal cells in the mouse. 3 Increased expression of NFIB mRNA in granulocytes has been described in PV, 13 which may suggest a compensatory or antagonist function of NFIB.…”

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confidence: 99%

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Alterations of NFIA in chronic malignant myeloid diseases

et al. 2008

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confidence: 99%

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Alterations of NFIA in chronic malignant myeloid diseases

et al. 2008

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“…Some years later, Lu et al proposed the causal association between this malformation syndrome and Nuclear Factor 1 A (NFIA) haplo-insufficiency [17]. NFIA maps on 1p31.2, carries 11 exons and produces at least 9 different protein isoforms [18][19][20].…”

Section: Introductionmentioning

confidence: 99%

CANPMR Syndrome and Chromosome 1p32-p31 Deletion Syndrome Coexist in Two Related Individuals Affected by Simultaneous Haplo-insufficiency of CAMTA1 and NIFA Genes

et al. 2016

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Background: Non-progressive cerebellar ataxia with mental retardation (CANPMR, OMIM 614756) and chromosome 1p32-p31 deletion syndrome (OMIM 613735) are two very rare inherited disorders, which are caused by mono-allelic deficiency (haplo-insufficiency) of calmodulin-binding transcription activator 1 (CAMTA1) and, respectively, nuclear factor 1 A (NFIA) genes. The yet reported patients affected by mono-allelic CAMTA1 dysfunction presented with neonatal hypotonia, delayed and ataxic gait, cerebellar atrophy, psychological delay and speech impairment, while individuals carrying a disrupted NFIA allele suffered from agenesis/hypoplasia of the corpus callosum, ventriculomegaly, developmental delay and urinary tract abnormalities. Both disorders were not seen in one patient together before. Results: In this study two related individuals affected by a complex clinical syndrome, characterized by cognitive, neurological and nephrological features were studied for the underlying genetic disorder(s) by molecular cytogenetics. The two individuals present dysmorphic facies, macrocephaly, generalized ataxia, mild tremor, strabismus, mild mental retardation and kidney hypoplasia. Moreover, neuro-radiological studies showed hypoplasia of corpus callosum. Genetic investigations revealed a paracentric inversion in the short arm of one chromosome 1 with breakpoints within CAMTA1 and NFIA coding sequences. Conclusions: To the best of our knowledge, this is the first report of two patients harboring the simultaneous mono-allelic disruptions and consequent haplo-insufficiencies of two genes due to an inversion event. Disruption of CAMTA1 and NFIA genes led to neuro-psychological and nephrological dysfunctions, which comprised clinical features of CANPMR syndrome as well as chromosome 1p32-p31 deletion syndrome.

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“…The latter might be related to the more severe phenotype seen in patients with NFIA deletions and in knockout mice, both showing malformations of the central nervous system. 7,8 It therefore seems that NFIA has a large number of functions, which is plausible for its role as a transcription factor.…”

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confidence: 99%