Modulating  gene expression to treat diseases

Matharu, Navneet

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Introduction
Programmable DNA targeting modules
Effector domains: transcription modulators
Fusions with effector domains
Human disease and transcriptional dosage
Haploinsufficiency
Zygosity of pathogenic genes
Around 15% of our genes could be haploinsufficient
Treatments for haploinsufficient disease
AAV vectors have a 4.7Kb limit on cargo
Transcriptional modulation-dCas9-fusions
Can CRISPRa correct haplinsufficiency?
Haploinsufficiency of SIM1 leads to obesity
SIM1 is downstream of the Leptin-Mc4r pathway
CRISPRa targeting to rescue Sim1 obesity
CRISPRa upregulates Sim1 in vitro
Sim1 CRISPRa upregulation strategy: in vivo
Sim1 promoter CRISPRa rescues obesity
Sim1 enhancer CRISPRa rescues obesity
Sim1 CRISPRa targeting can define tissue specificity
CRISPRa-AAV upregulates Sim1 in the hypothalamus
Postnatal rescue of neuroendocrine obesity
Sim1-CRISPRa-AAVs have long lasting effect
Can CRISPRa strategy work for other HI genes?
Leptin-Mc4r pathway
CRISPRa-AAV rescues Mc4r haploinsufficiency
Overcoming size limitation of AAV gene therapy
Summary
Loss of function of Lama2-MDC1A
CRISPRa targeting alternative/redundant gene
FABP4 expression is linked to many diseases
CRISPRi to downregulate the biomarker genes
Autosomal dominant: Huntington's Disease
ZF-KRAB to downregulate the pathogenic gene
DNA methylation modulation
DNA looping modulation
Advantages and disadvantages
Acknowledgements

Topics Covered

Programmable DNA targeting modules
Effector domain functions and possibilities
Haploinsufficiency and its role in disease
CRISPRa targeting strategy to rescue Sim1 obesity
CRISPRa targeting strategy to treat Mc4r haploinsufficiency

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Periodic Reports: Advances in Clinical Interventions and Research Platforms

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Talk Citation

Matharu, N. (2021, December 13). Modulating gene expression to treat diseases [Video file]. In The Biomedical & Life Sciences Collection, Henry Stewart Talks. Retrieved November 20, 2024, from https://doi.org/10.69645/BOTL2560.
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Publication History

Published on December 13, 2021

Financial Disclosures

Dr. Navneet Matharu has not informed HSTalks of any commercial/financial relationship that it is appropriate to disclose.

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Modulating gene expression to treat diseases

Dr. Navneet Matharu – University of California San Francisco, USA

Published on December 13, 2021 20 min

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Transcript

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0:00

Hi, everybody. This is Navneet Matharu; I'm an Assistant Professor in the Department of Bioengineering and Therapeutic Sciences at UCSF. The topic of my talk today is future gene therapy strategies for modulating gene expression. It's my pleasure to discuss with you today some of the recent advances in research that highlight the use of non-editing versions of gene editors to treat genetic disorders.

0:28

Broadly, there are three versions of gene editors that are explored in the last couple of decades first-generation: zinc-finger nucleases, second-generation: TALENs, and third-generation: the CRISPR system. All of these have programmable DNA recognition or targeting modules. Zinc finger nucleases have C2H2 zinc-finger domains for DNA recognition. TALENs have TAL effector DNA recognition and binding domains and CRISPR is a ribonuclease complex where DNA target recognition is guided by the guide, RNA. Zinc fingers or TALs can be made into nucleases by fusing the FOK1 restriction enzyme that creates a single-strand DNA break. It takes two zinc-finger FOK when fusion molecules to make a double-strand DNA break. CRISPR-Cas9 mind hazard to new peers domains that can make double-stranded DNA break. These editors can be programmed into nuclease deficient versions, for example, if you don't fuse a FOK1 to zinc-finger or TAL these molecules are nucleus deficient on their own. To make nuclease deficient CRISPR Cas9 we can mutate these two catalytically active nucleus domains such that it loses its DNA editing ability and we can make a dead Cas9 version out of it. Now, these DNA targeting modules can be fused to any effective domains that can perform a variety of biochemical functions at the target locus. These effector domains that can modulate the target gene expression are mostly transcription activators or repressors.

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