Alternative splicing in human myeloid cell differentiation and leukaemia

Dysregulation of alternative splicing (AS) has been implicated in aberrant cell function, resulting in diseases such as acute myeloid leukaemia (AML). It was found that myeloid cell differentiation was impaired due to mutations and altered expression levels of splicing factors (SFs). Preliminary dat...

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Main Author:	Lim, Kai Yi
Other Authors:	Francesc Xavier Roca Castella
Format:	Final Year Project
Language:	English
Published:	Nanyang Technological University 2021
Subjects:	Science::Biological sciences::Molecular biology Science::Biological sciences::Genetics
Online Access:	https://hdl.handle.net/10356/153292
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Institution:	Nanyang Technological University
Language:	English

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spelling	sg-ntu-dr.10356-1532922023-02-28T18:01:15Z Alternative splicing in human myeloid cell differentiation and leukaemia Lim, Kai Yi Francesc Xavier Roca Castella School of Biological Sciences xroca@ntu.edu.sg Science::Biological sciences::Molecular biology Science::Biological sciences::Genetics Dysregulation of alternative splicing (AS) has been implicated in aberrant cell function, resulting in diseases such as acute myeloid leukaemia (AML). It was found that myeloid cell differentiation was impaired due to mutations and altered expression levels of splicing factors (SFs). Preliminary data has shown RNA-binding motif protein 47 (RBM47) to be one of the upregulated SFs in AML cells. In this study, effect of RBM47 expression levels on myeloid cell differentiation was studied using HL-60 as a differentiation model. HL-60 overexpressing RBM47 was differentiated alongside wild-type and the extent of differentiation was measured and compared. We found that RBM47 overexpression in differentiating HL-60 cells increased surface expression of maturation markers, elevated baseline ROS levels and improved phagocytic ability. Meanwhile, overexpressing RBM47 did not alter untreated, undifferentiated cells. RBM47-regulation of AS in HL-60 was also investigated, and we report that inclusion of exon 12 in MAP3K7 mRNA was induced by RBM47. Findings of this study suggest that RBM47 overexpression supports myeloid cell differentiation by accelerating the process after initiation by other factors. It is possible that RBM47 achieves this effect through AS of several key genes in cell differentiation, though more work is required before conclusions can be drawn. Bachelor of Science in Biological Sciences 2021-11-17T06:58:02Z 2021-11-17T06:58:02Z 2021 Final Year Project (FYP) Lim, K. Y. (2021). Alternative splicing in human myeloid cell differentiation and leukaemia. Final Year Project (FYP), Nanyang Technological University, Singapore. https://hdl.handle.net/10356/153292 https://hdl.handle.net/10356/153292 en application/pdf Nanyang Technological University
institution	Nanyang Technological University
building	NTU Library
continent	Asia
country	Singapore Singapore
content_provider	NTU Library
collection	DR-NTU
language	English
topic	Science::Biological sciences::Molecular biology Science::Biological sciences::Genetics
spellingShingle	Science::Biological sciences::Molecular biology Science::Biological sciences::Genetics Lim, Kai Yi Alternative splicing in human myeloid cell differentiation and leukaemia
description	Dysregulation of alternative splicing (AS) has been implicated in aberrant cell function, resulting in diseases such as acute myeloid leukaemia (AML). It was found that myeloid cell differentiation was impaired due to mutations and altered expression levels of splicing factors (SFs). Preliminary data has shown RNA-binding motif protein 47 (RBM47) to be one of the upregulated SFs in AML cells. In this study, effect of RBM47 expression levels on myeloid cell differentiation was studied using HL-60 as a differentiation model. HL-60 overexpressing RBM47 was differentiated alongside wild-type and the extent of differentiation was measured and compared. We found that RBM47 overexpression in differentiating HL-60 cells increased surface expression of maturation markers, elevated baseline ROS levels and improved phagocytic ability. Meanwhile, overexpressing RBM47 did not alter untreated, undifferentiated cells. RBM47-regulation of AS in HL-60 was also investigated, and we report that inclusion of exon 12 in MAP3K7 mRNA was induced by RBM47. Findings of this study suggest that RBM47 overexpression supports myeloid cell differentiation by accelerating the process after initiation by other factors. It is possible that RBM47 achieves this effect through AS of several key genes in cell differentiation, though more work is required before conclusions can be drawn.
author2	Francesc Xavier Roca Castella
author_facet	Francesc Xavier Roca Castella Lim, Kai Yi
format	Final Year Project
author	Lim, Kai Yi
author_sort	Lim, Kai Yi
title	Alternative splicing in human myeloid cell differentiation and leukaemia
title_short	Alternative splicing in human myeloid cell differentiation and leukaemia
title_full	Alternative splicing in human myeloid cell differentiation and leukaemia
title_fullStr	Alternative splicing in human myeloid cell differentiation and leukaemia
title_full_unstemmed	Alternative splicing in human myeloid cell differentiation and leukaemia
title_sort	alternative splicing in human myeloid cell differentiation and leukaemia
publisher	Nanyang Technological University
publishDate	2021
url	https://hdl.handle.net/10356/153292
_version_	1759854096940007424

Alternative splicing in human myeloid cell differentiation and leukaemia

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