Publications by authors named "Teresa Puchner"
Genetic networks are characterized by extensive buffering. During tumor evolution, disruption of functional redundancies can create de novo vulnerabilities that are specific to cancer cells. Here, we systematically search for cancer-relevant paralog interactions using CRISPR screens and publicly available loss-of-function datasets.
View Article and Find Full Text PDFAberrant WNT pathway activation, leading to nuclear accumulation of β-catenin, is a key oncogenic driver event. Mutations in the tumor suppressor gene APC lead to impaired proteasomal degradation of β-catenin and subsequent nuclear translocation. Restoring cellular degradation of β-catenin represents a potential therapeutic strategy.
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- The study reveals a new dependency of SMARCA4 in esophageal squamous cell carcinoma (ESCC) models lacking SMARCA2, contrary to the previously known synthetic lethal relationship in SMARCA4-deficient cancers.* -
- Restoration of SMARCA2 expression reduces reliance on SMARCA4, whereas loss of SMARCA2 increases vulnerability to SMARCA4 depletion, highlighting the importance of SMARCA4's ATPase activity.* -
- The research proposes targeting SMARCA4 as a promising therapeutic strategy for cancers deficient in SMARCA2, expanding the understanding of their interaction and potential drug development avenues.*
Bile acids are established signaling molecules next to their role in the intestinal emulsification and uptake of lipids. We here aimed to identify a potential interaction between bile acids and CD4+ Th cells, which are central in adaptive immune responses. We screened distinct bile acid species for their potency to affect T cell function.
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