2020
DOI: 10.1186/s12868-020-00577-1
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Hcfc1a regulates neural precursor proliferation and asxl1 expression in the developing brain

Abstract: Background Precise regulation of neural precursor cell (NPC) proliferation and differentiation is essential to ensure proper brain development and function. The HCFC1 gene encodes a transcriptional co-factor that regulates cell proliferation, and previous studies suggest that HCFC1 regulates NPC number and differentiation. However, the molecular mechanism underlying these cellular deficits has not been completely characterized. Methods Here we crea… Show more

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Cited by 9 publications
(13 citation statements)
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References 63 publications
(131 reference statements)
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“…In addition, we designed a splice inhibiting morpholino to the 3′ splice acceptor of exon 2, but the designed morpholino did not delete exon 3 as predicted, even at the highest concentration injected (2 nl of a 0.9 mM stock solution). We did, however, utilize a random control morpholino to account for the possibility of morpholino-induced cell death, an endeavor that proved to be rather successful in previous studies [ 54 , 55 ]. And, while injection of HS side chains is a potential rescue for the morphant phenotype we observe, there is the possibility that HS/heparin co-injection would fail to rescue because a domain outside of domain I is also essential for regulation of CNCCs.…”
Section: Discussionmentioning
confidence: 99%
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“…In addition, we designed a splice inhibiting morpholino to the 3′ splice acceptor of exon 2, but the designed morpholino did not delete exon 3 as predicted, even at the highest concentration injected (2 nl of a 0.9 mM stock solution). We did, however, utilize a random control morpholino to account for the possibility of morpholino-induced cell death, an endeavor that proved to be rather successful in previous studies [ 54 , 55 ]. And, while injection of HS side chains is a potential rescue for the morphant phenotype we observe, there is the possibility that HS/heparin co-injection would fail to rescue because a domain outside of domain I is also essential for regulation of CNCCs.…”
Section: Discussionmentioning
confidence: 99%
“…AVMA guidelines for embryos younger than 7 DPF were followed, which indicate 1–10% sodium hypochlorite solution following anesthesia. Detailed methods for anesthesia and euthanasia have been previously described [ 54 ].…”
Section: Methodsmentioning
confidence: 99%
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“…In addition, we designed a splice inhibiting morpholino to the 3' splice acceptor of exon 2, but the designed morpholino did not delete exon 3 as predicted, even at the highest concentration injected (2nl of a 0.9mM stock solution). We did, however, utilize a random control morpholino to account for the possibility of morpholino-induced cell death, an endeavor that proved to be rather successful in previous studies (54,55). And, while injection of HS side chains is a potential rescue for the morphant phenotype we observe, there is the possibility that HS/heparin coinjection would fail to rescue because a domain outside of domain I is also essential for regulation of CNCCs.…”
Section: Discussionmentioning
confidence: 98%
“…For all experiments, the morphant experimental group is compared to either a random control group or wildtype non-injected. The randomized control morpholino has been shown through previous literature to have no associated phenotypes, indicating that it does not in uence nal results and therefore is the appropriate control group for comparison (54,55,57). Thus, for statistical analysis, comparisons were performed using a T-test between the random control group and the morpholino.…”
Section: Antisense Oligonucleotide Morpholino Design and Microinjectionmentioning
confidence: 99%