1. What contributions have the authors mentioned in the paper "Comprehensive genotyping and clinical characterisation reveal 27 novel nkx2-1 mutations and expand the phenotypic spectrum" ?
In this paper, Anne Thorwarth, Sarah Schnittert-Hübener, Pamela Schrumpf, Ines Müller, Sabine Jyrch, Christof Dame, Heike Biebermann, Gunnar Kleinau, Juri Katchanov, Markus Schuelke, Grit Ebert, Anne Steininger, Carsten Bönnemann, Knut Brockmann, Hans-Jürgen Christen, Patricia Crock, Francis deZegher, Matthias Griese, Jacqueline Hewitt, Sten Ivar
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2. What future works have the authors mentioned in the paper "Comprehensive genotyping and clinical characterisation reveal 27 novel nkx2-1 mutations and expand the phenotypic spectrum" ?
This may impact the use of congenital NKX2-1 mutations as a prognostic marker in future.. There, only nonsense or frame-shift mutations in the N-terminal part, and potentially also in the C-terminal part,37 can compromise protein functionality.. 75 Noteworthy, HOP, one of the shared downstream targets of NKX2-1 and NKX2-5 ( see above ), is a homeodomain protein that lacks any DNA binding potential.. 78 79 For one of these conserved sequences, a forebrain expression has already been shown ( http: //enhancer. lbl. gov/cgi-bin/ imagedb3. pl ? form=presentation & show=1 & experiment_id=1538 & organism_id=1 ) and the other one has been highlighted as potential enhancer by a recent meta-analysis of GWAS data related to thyroid function and TSH levels.
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3. How many deletions were identified in the NKX2-1 genome?
By using a 44k customised oligonucleotide array, the authors identified 10 heterozygous deletions affecting the chromosomal region 14q13 in 10 patients.
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4. What are the two genes that are not mentioned in the context of CNVs?
Two genes recently discussed in the context of CNVs outside NKX2-1 are NPAS3 and RALGAPA1.77 Malfunction of these two genes can lead to respiratory distress and cognitive disorders, respectively.
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![Figure 5 Additional symptoms in patients with NKX2-1 mutations. (A) Body height standard deviation score (SDS) values of detailed phenotype cohort. Median value −0.84 SDS; patients 1–18 carrying NKX2-1 mutations: 1, chr14:g (36042742_36142540)del; 2, chr14:g (36042742_36142540)del; 3, chr14:g (36042742_36142540)del; 4, chr14:g (35138127_37502915)del; 5, chr14:g (32446471_41666818)del; 6, chr14:g (31766511_46944545)del; 7, chr14:g (35883857_38226260)del; 8, c.522C>G_p.Tyr174X; 9, c.522C>G_p. Tyr174X; 10, c.585nsGG_p. Leu195GlyfsX3; 11, c.613G>T_p. Val205Phe; 12, [c.608C>G] +[c.613G>T]_[p.Thr203Arg]+[p. Val205Phe]; 13, c.608C>G_p. Val205Phe; 14, c.608C>G_p. Val205Phe; 15, c.608C>G_p. Val205Phe; 16, c.338G>A_p.Trp113X; 17, c.261C>A_p.Cys87X; 18, c.261C>A_p.Cys87X; 19, c.506C>A_p. Ser169X; 20, c.157insC_p. Met53HisfsX355; 21, c.236C>A_p. Ser79X; 22, c.236C>A_p.Ser79X; 23, c.236C>A_p.Ser79X; 24, c.866_883delinsCTACA_p. Gln289ProfsX59; 25, c.793delA_p. Lys265LysfsX87;26, c.712delGG_p. Gly238ArgfsX170; 27, c.712delGG_p. Gly238ArgfsX170; 28, c.339delG_p. Trp113CysfsX16. (B) Heatmap summarising the results of detailed phenotyping in 18 index patients and 10 relatives with NKX2-1 deficiency. The presence and absence of symptoms is indicated by yellow and blue boxes, respectively. Missing values are shown in grey. The first seven columns to the left depict the phenotypes of the patients affected by a copy number variant. Point mutations are sorted according to their genomic position. The letters (a), (b) and (c) heading the description of the mutation indicate family members sharing the same mutation.](/figures/figure-5-additional-symptoms-in-patients-with-nkx2-1-15g6gydp.webp)
