Dyskeratosis

Overview of Dyskeratosis

Most recent studies have shown that Dyskeratosis shares some biological mechanisms with acantholysis, anemia, aplastic-anemia, carcinoma, dermatologic-disorders, dyskeratosis-congenita, dystrophia-unguium, dystrophy, hyperkeratosis, keratosis, keratosis-follicularis, leukoplakia, leukoplakia-oral, malignant-neoplasms, neoplasms, pancytopenia, pigmentation-disorders, skin-neoplasms, telomere-shortening, x-linked-dyskeratosis-congenita.

Among the many pathways, these few ones have gauged particular interests from scientists studying Dyskeratosis, and have been seen in publications frequently: Aging, Cell Cycle, Cell Death, Cell Division, Cell Proliferation, Cellular Senescence, Cornification, Dna Repair, Dna Replication, Hypersensitivity, Keratinization, Localization, Pathogenesis, Pigmentation, Ribosome Biogenesis, Rna Modification, Rna Processing, Senescence, Telomere Maintenance, Translation

Quite a number of genes have been found to play important roles in Dyskeratosis, such as ASAP2, ATP2A2, CSF3, DCX, DKC1, FANCA, FXN, GAR1, MRPS30, NHP2, NOP10, PAPOLA, RNPC3, TERT, TINF2, TP53. See what Boster has to offer for the research of these genes by clicking the gene name links below and view a more detailed info card/product listing for that gene.

In a later update, we will include information such as current drugs and therapy solutions as well as on-going and past clinical trials for this disease. Plesae stay updated.

Dyskeratosis Related Genes

click to see detail information for each gene

Pathways Related to Dyskeratosis

This information is being compiled and will come in a future update

Related Diseases