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The Walleye dermal sarcoma virus cyclin causes excessive skin cell growth in mice.

Skin cancer often starts from Lgr5+ progenitor cells.

Overexpressing ATF3 in mice's epithelial cells may lead to oral cancer.

Oncogenic K-ras causes rapid cancerous changes in the mouth's lining.

Deleting Smad4 and PTEN genes in mice causes rapid, invasive stomach cancer.

Deleting Smad4 and PTEN genes in mice causes rapid, invasive forestomach cancer.

The skin and thymus develop similarly to protect and support immunity.

PRF lysates reduce inflammation in cancer cells and boost immune response in healthy oral cells.

Sox9 is present in most canine skin tumors and may help understand stem cells' role in these cancers.

The Apc gene is crucial for normal skin and thymus development.

New treatments targeting specific genes show promise for treating keratin disorders.

Skin abnormalities can indicate immunodeficiency due to shared origins with the immune system.

RSPO1 mutations in certain patients lead to skin cells that don't develop properly and are more likely to become invasive, increasing the risk of skin cancer.

Understanding where cancer cells come from helps create better prevention and treatment methods.

Matriptase is crucial for skin barrier, hair growth, and may contribute to skin cancer.

HPV genes and estradiol increase a cancer-related signaling pathway, which may be targeted for cervical cancer treatment.

Older skin has higher cancer risk due to inflammation and stem cell issues.

Bone marrow and hair follicle cells help form skin tumors, suggesting new treatment targets.

Bone marrow-derived cells contribute to skin tumors, suggesting new treatment targets for non-melanoma skin cancers.

The document concludes that individualized treatment for malignant epithelial tumors is necessary and more research on metastatic squamous cell carcinoma treatments is needed.

Orai1 protein is crucial for tooth development and affects enamel thickness and mineralization.

Loss of TET2 increases the risk of skin and oral cancer.

A WNT10A gene mutation leads to ectodermal dysplasia by disrupting cell growth and differentiation.

Keratin 75 might be important in oral cancer progression.

Targeting the p63 gene could help treat skin diseases.

OCT can effectively screen and diagnose various medical conditions non-invasively.

SVpgC2a cells show abnormal growth and keratin changes, modeling early cancer development.

Understanding molecular processes in skin development is key to creating targeted treatments for skin disorders.

Photodynamic therapy may not work for erythroplasia of Queyrat and could lead to invasive squamous cell carcinoma.

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