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Keratinocyte cytokines and genetic variations influence the development of moles and skin pigmentation.

Melanocyte pathology requires keratinocyte hyperplasia and regulation dysfunction.

Matrical tumors share a common growth mechanism involving the Wnt pathway and consistent PHLDA1 expression.

PNKP is essential for keeping adult mouse progenitor cells healthy and growing normally.

The mTOR pathway may be involved in the development of hair follicle tumors, with higher activity in malignant tumors.

Passage numbers affect cell growth and experiment results.

Imaging intestinal stem cells might help detect early signs of colorectal cancer.

A mutation in the MAP2 gene causes reduced hair follicle density, leading to hairlessness.

Identical p53 gene mutations in different cancers suggest the need for careful treatment.

KIF18B is important for correctly positioning cell division machinery in skin cells, affecting hair follicle development.

A new imaging technique can observe stem cells in living mice without harming them.

Inhibiting mTORC2 can reduce DNA repair and increase cancer cell death, suggesting potential for targeted brain cancer treatments.

PKC ε increases hair follicle stem cell turnover and may raise skin cancer risk.

Increasing SSAT makes skin more prone to cancer.

MTS24 marks a new type of skin cell that helps hair growth and repair.

PTCH gene mutations contribute to basal cell carcinoma development.

Changing CDK4 levels affects the number of stem cells in mouse hair follicles.

Activating β-catenin in mammary cells leads to changes that cause early-stage abnormal growths similar to skin structures.

Loss of the p53 gene alone causes tumors, and losing both p53 and Rb genes speeds up aggressive skin cancer.

The study found that analyzing certain cell signaling pathways is not a reliable method to tell apart two types of skin tumors.

Mutations in the SHH pathway in certain skin cells can cause skin tumors and abnormal hair growth.

Cancer can hijack the body's cell repair system to promote tumor growth, and targeting this process may improve cancer treatments.

mrp/plf-mRNA can indicate tumor-promoting effects in skin.

YAP and TAZ proteins are necessary for the development of two types of skin cancer.

AP-1 and TGFß work together to drive resistance in basal cell carcinoma, suggesting new treatment options.

Inactivating both p53 and Rb genes in mice speeds up aggressive skin cancer development.

The gene p53 is crucial for removing damaged cells to allow for healthy tissue renewal.

Loss of the p53 gene alone causes tumors, and losing both p53 and Rb genes speeds up aggressive skin cancer.

The document concludes that DNA methylation and the mTOR pathway are important for stem cell function and could impact disease treatment.

Blocking the Mitochondrial Pyruvate Carrier causes stress in hair follicles, which can be reduced by an ISR inhibitor.