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Normal human melanocytes can avoid cell death through multiple pathways.

The study identified a key protein involved in producing underarm odor and found ways to inhibit it.

Autophagy is crucial for normal sebaceous gland function and sebum composition.

Human TMEM2 does not break down hyaluronan but helps control its metabolism.

2-Methoxyestradiol causes cancer cell death by activating specific pathways, but androgens can block this effect.

Cystatin M/E strongly inhibits cathepsin V and cathepsin L, important for skin formation.

Two distinct caspases in human skin help with cell death and skin formation.

A molecule called α-ketobutyrate was found to extend lifespan and improve aging-related symptoms in worms and mice by activating certain cellular pathways and may help develop anti-aging treatments for humans.

Hairless protein and putrescine regulate each other, affecting hair growth and skin balance.

Loss of the Y chromosome and UTY gene activity increases cancer risk in men.

Ulcerative colitis involves immune activation, chronic inflammation, and metabolic issues, some of which persist even during remission.

Proteolytic enzymes damage hair follicles by detaching stem cells.

Catalytic antibodies are early indicators and active participants in the development of systemic lupus erythematosus.

Blocking specific proteins can help remove aging cells and might treat age-related diseases and promote hair growth.

Activating mitophagy may help manage a key immune response involved in the hair loss condition alopecia areata.

Proteolytic enzymes damaged hair follicle stem cells in transgenic mice.

UTX is important for skin health and its loss can lead to skin issues, especially in females.

Blocking autophagy worsens lipid buildup and dysfunction in brain cells after injury.

NCSTN gene mutation causes abnormal skin cell differentiation and more inflammation, contributing to Hidradenitis Suppurativa.

QSOX enzymes help form protein bonds in cells, especially in tissues with high secretory activity.

A gene mutation in mice causes hair loss, weak bones, and protein buildup, showing how protein processing issues can lead to diseases.

Activating autophagy might reverse skin fibrosis.

ERULUS controls root hair growth by regulating cell wall composition and pectin activity.

Overexpression of hurpin in mice leads to abnormal skin and higher skin cancer risk.

The document concludes that the discussed biological mechanisms and potential therapies are not related to hair loss or hair growth.

Defective protein folding due to a mutation is key in ANE syndrome.

MOF controls skin development by regulating genes for mitochondria and cilia.

A protein called PCBP2 controls the production of a hair growth protein by interacting with its genetic message and is linked to hair loss when this control is disrupted.