Warning: Undefined array key "mm" in /www/wwwroot/www.ai-bt.com/si.php on line 10 Deprecated: trim(): Passing null to parameter #1 ($string) of type string is deprecated in /www/wwwroot/www.ai-bt.com/si.php on line 10 CRISPR/Cas9-Mediated Point Mutation in Nkx3.1 Prolongs Protein Half-Life and Reverses Effects Nkx3.1 Allelic Loss.

Literature DB >> 32943441

CRISPR/Cas9-Mediated Point Mutation in Nkx3.1 Prolongs Protein Half-Life and Reverses Effects Nkx3.1 Allelic Loss.

Cai Bowen¹, Maho Shibata¹, Hailan Zhang², Sarah K Bergren¹, Michael M Shen¹, Edward P Gelmann³.

Abstract

NKX3.1 is the most commonly deleted gene in prostate cancer and is a gatekeeper suppressor. NKX3.1 is haploinsufficient, and pathogenic reduction in protein levels may result from genetic loss, decreased transcription, and increased protein degradation caused by inflammation or PTEN loss. NKX3.1 acts by retarding proliferation, activating antioxidants, and enhancing DNA repair. DYRK1B-mediated phosphorylation at serine 185 of NKX3.1 leads to its polyubiquitination and proteasomal degradation. Because NKX3.1 protein levels are reduced, but never entirely lost, in prostate adenocarcinoma, enhancement of NKX3.1 protein levels represents a potential therapeutic strategy. As a proof of principle, we used CRISPR/Cas9-mediated editing to engineer in vivo a point mutation in murine Nkx3.1 to code for a serine to alanine missense at amino acid 186, the target for Dyrk1b phosphorylation. Nkx3.1S186A/-, Nkx3.1+/- , and Nkx3.1+/+ mice were analyzed over one year to determine the levels of Nkx3.1 expression and effects of the mutant protein on the prostate. Allelic loss of Nkx3.1 caused reduced levels of Nkx3.1 protein, increased proliferation, and prostate hyperplasia and dysplasia, whereas Nkx3.1S186A/- mouse prostates had increased levels of Nkx3.1 protein, reduced prostate size, normal histology, reduced proliferation, and increased DNA end labeling. At 2 months of age, when all mice had normal prostate histology, Nkx3.1+/- mice demonstrated indices of metabolic activation, DNA damage response, and stress response. These data suggest that modulation of Nkx3.1 levels alone can exert long-term control over premalignant changes and susceptibility to DNA damage in the prostate. SIGNIFICANCE: These findings show that prolonging the half-life of Nkx3.1 reduces proliferation, enhances DNA end-labeling, and protects from DNA damage, ultimately blocking the proneoplastic effects of Nkx3.1 allelic loss. ©2020 American Association for Cancer Research.

Entities: CellLine Chemical Disease Gene Mutation Species

Mesh：

Substances：

Year: 2020 PMID： 32943441 PMCID： PMC7642110 DOI： 10.1158/0008-5472.CAN-20-1742

Source DB: PubMed Journal: Cancer Res ISSN： 0008-5472 Impact factor: 12.701

Keyword Cloud
References

52 in total

1. Integrative genomic profiling of human prostate cancer.

Authors: Barry S Taylor; Nikolaus Schultz; Haley Hieronymus; Anuradha Gopalan; Yonghong Xiao; Brett S Carver; Vivek K Arora; Poorvi Kaushik; Ethan Cerami; Boris Reva; Yevgeniy Antipin; Nicholas Mitsiades; Thomas Landers; Igor Dolgalev; John E Major; Manda Wilson; Nicholas D Socci; Alex E Lash; Adriana Heguy; James A Eastham; Howard I Scher; Victor E Reuter; Peter T Scardino; Chris Sander; Charles L Sawyers; William L Gerald
Journal: Cancer Cell Date: 2010-06-24 Impact factor: 31.743

2. Deletion, methylation, and expression of the NKX3.1 suppressor gene in primary human prostate cancer.

Authors: Ekatherine Asatiani; Wen-Xin Huang; Antai Wang; Elizabeth Rodriguez Ortner; Luciane R Cavalli; Bassem R Haddad; Edward P Gelmann
Journal: Cancer Res Date: 2005-02-15 Impact factor: 12.701

3. Structural and functional analysis of domains mediating interaction between the bagpipe homologue, Nkx3.1 and serum response factor.

Authors: Yan Zhang; Rebecca A Fillmore; Warren E Zimmer
Journal: Exp Biol Med (Maywood) Date: 2008-03

10. Systems analysis of the prostate tumor suppressor NKX3.1 supports roles in DNA repair and luminal cell differentiation.

Authors: Chih-Cheng Yang; Alicia Chung; Chia-Yu Ku; Laurence M Brill; Roy Williams; Dieter A Wolf
Journal: F1000Res Date: 2014-05-21

CRISPR/Cas9-Mediated Point Mutation in Nkx3.1 Prolongs Protein Half-Life and Reverses Effects Nkx3.1 Allelic Loss.

1. Integrative genomic profiling of human prostate cancer.

2. Deletion, methylation, and expression of the NKX3.1 suppressor gene in primary human prostate cancer.

3. Structural and functional analysis of domains mediating interaction between the bagpipe homologue, Nkx3.1 and serum response factor.

4. Oxidative DNA damage induced by nitrotyrosine, a biomarker of inflammation.

5. Structural and functional interactions of the prostate cancer suppressor protein NKX3.1 with topoisomerase I.

6. Inflammatory cytokines induce phosphorylation and ubiquitination of prostate suppressor protein NKX3.1.

7. Ligand-dependent enhancer activation regulated by topoisomerase-I activity.

8. Identification of programmed cell death in situ via specific labeling of nuclear DNA fragmentation.

9. Antioxidant treatment promotes prostate epithelial proliferation in Nkx3.1 mutant mice.

10. Systems analysis of the prostate tumor suppressor NKX3.1 supports roles in DNA repair and luminal cell differentiation.