Project Summary/Abstract The tumor suppressor p53 is often referred to as the “guardian of the genome”. Mutations of the p53 gene occur in ~50% of human cancer and loss of p53 function is known to play a central role in tumor progression and metastasis. Upon exposure to a stress signal, such as DNA damage, p53 transcription factor is activated and then induces an array of pro-survival and pro-death genes. Due to its potent role in tumor suppression, p53 is an attractive target for the development of new anticancer drugs. Nerve injury-induced protein 1 (Ninjurin1, NINJ1) and NINJ2 constitute the Ninjurin family of cell adhesion molecules and have been implicated in various pathological processes such as immune response. However, the role of NINJ1 and NINJ2 in tumorigenesis is unclear. We showed previously that NINJ1 is a target of p53 and in turn represses p53 mRNA translation. Thus, NINJ1 and p53 forms a negative feedback loop. Notably, our pilot study showed that NINJ1 and NINJ2 interact with each other through their N-terminal extracellular domains. We also found that like NINJ1, NINJ2 forms a negative regulatory loop with p53. To determine the biological significance of the NINJ1-NINJ2-p53 loop, we showed that: (1) loss of NINJ1 or NINJ2 inhibits cell migration and formation of tumor spheres and colonies in breast cancer cells and promote cellular senescence in mouse embryonic fibroblasts in a p53- dependent manner; (2) mice deficient in Ninj1 or Ninj2 are prone to chronic inflammation, which is likely due to enhanced pyroptosis through wild-type p53-dependent activation of NLRP3 inflammasome; (3) two small peptides, called Pep-1A and Pep-2A derived from N-terminal alpha helix domain of NINJ1 and NINJ2 protein were able to disrupt the formation of NINJ1-NINJ2 complex and elicit growth suppression. These observations prompt us to hypothesize that both NINJ1 and NINJ2 play a critical role in tumorigenesis through the p53 pathway. To test this, we will determine: (1) the feedback regulatory loops between NINJ1 and NINJ2 and between p53 and the Ninjurin family; (2) the biological significance of the NINJ1-NINJ2-p53 loop in tumor suppression; (3) whether the Ninj1- Ninj2-p53 loop can be targeted to kill tumor cells carrying wild-type p53.