Research Day 1 (Monday, May 12, 2025)

Suppression of stress granule formation is a novel vulnerability imposed by mutant p53

Elizabeth Thoenen, Children's Mercy Kansas CityFollow
Atul Ranjan, Children's Mercy Kansas CityFollow
Alejandro Parrales, Children's Mercy Kansas CityFollow
Shigeto Nishikawa, Kyoto UniversityFollow
Dan A. Dixon, University of Arkansas for Medical SciencesFollow
Sugako Oka, Kyushu UniversityFollow
Tomoo Iwakuma, Children's Mercy Kansas CityFollow

Presenter Status

Resident/Ph.D/Post graduate (> 1 month of dedicated research time)

Abstract Type

Research

Primary Mentor

Tomoo Iwakuma

Start Date

12-5-2025 11:30 AM

End Date

12-5-2025 1:30 PM

Presentation Type

Poster-Restricted Access

Description

The main objective of this study was to identify how mutp53 inhibits ER-stress induced SG formation in HCC, leading to apoptosis.

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May 12th, 11:30 AM May 12th, 1:30 PM

Suppression of stress granule formation is a novel vulnerability imposed by mutant p53

The main objective of this study was to identify how mutp53 inhibits ER-stress induced SG formation in HCC, leading to apoptosis.

Research Day 1 (Monday, May 12, 2025)

Suppression of stress granule formation is a novel vulnerability imposed by mutant p53

Presenter Status

Abstract Type

Primary Mentor

Start Date

End Date

Presentation Type

Description

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Research Day 1 (Monday, May 12, 2025)

Suppression of stress granule formation is a novel vulnerability imposed by mutant p53

Authors

Presenter Status

Abstract Type

Primary Mentor

Start Date

End Date

Presentation Type

Description

Restricted

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