Leukoencephalopathy

Watchlist

(log in to enable)

Retrieved

2021-01-18

Source

Wikipedia

Trials

—

Genes

CSF1R, COL4A1, TYMP, SCP2, SPP1, APP, TCN2, RHOA, MTHFR, MTR, DPYD, DARS2, BDNF, CDKN1B, NOTCH3, EIF2B2, EIF2B1, EIF2B4, CLCN2, DARS1, POLG, EIF2B5, SNORD118, RPIA, NDUFS1, NDUFAF3, HTRA1, L2HGDH, VPS11, GJC2, CLN6, TYROBP, COA8, NUBPL, EARS2, NAXE, NDUFV1, PLAA, NFE2L2, SAMHD1, NDUFS8, NDUFS6, NDUFS4, MRPS22, NDUFS3, NDUFS2, NDUFV2, TACO1, SCN8A, SCO1, YME1L1, PMPCB, AIFM1, NDUFAF1, RRM2B, TREX1, EIF2B3, NDUFB10, NDUFB11, TMEM70, FASTKD2, FOXRED1, TIMMDC1, KMT2E, NDUFAF4, TMEM126B, NDUFB9, MARS2, CTC1, PET100, AUH, NDUFS7, COX6B1, COX8A, COX10, B3GALNT2, NDUFA11, COX20, NDUFAF2, HMGCL, COX14, LAMB1, HIBCH, COLGALT1, ND2, TRNS1, ND3, NDUFAF5, NDUFA1, NDUFA6, TRNN, ND1, NDUFB3, AARS2, MLC1, EIF2S2, HEPACAM, SDHAF1, RNASET2, TUBB4A, ABCB6, LGALS14, GFAP, APOE, WARS2, CSF2, DEAF1, NFU1, PSEN1, LAMA2, KARS1, ISCA2, COA7, KCNT1, POLR3B, NOTCH2NLC, DDX59, SLC2A4RG, SHANK3, SLC26A5, GGCT, ACBD5, LYRM7, SLC5A8, RMND1, GLRX5, TREM2, MTFMT, IBA57, HIKESHI, SLC13A3, AARS1, SZT2, MS, MOG, MBP, MANBA, KIF5A, IL6, IFNG, IFNB1, HMGB1, HMBS, GJA1, GFPT1, FMR1, EIF2S3, EIF2S1, EEF1A1, EDN1, SARDH, CST3, COL4A2, CLCN1, C1QBP, ALDH3A2, ABCD1, JAG1, ADORA2A, MPV17, COX2, POLR3A, MYL2, SDS, MYL9, SCO2, FIG4, ARHGEF2, DEGS1, CUL4B, VEGFA, TUFM, TLR2, SURF1, ACTA2, SORD, SLC16A2, SLC2A1, SDHB, CCL5, PTGS2, PRPS1, PLP1, PDGFB, PAFAH1B1, NEFL, NDUFB8, NDUFA2, MTCO2P12

Drugs

—

Interested in hearing about new therapies?

Leukoencephalopathy (leukodystrophy-like diseases) is all of the brain white matter diseases, whether their molecular cause is known or not. It can refer specifically to any of these diseases:

Progressive multifocal leukoencephalopathy
Toxic leukoencephalopathy
Leukoencephalopathy with vanishing white matter
Leukoencephalopathy with neuroaxonal spheroids
Reversible posterior leukoencephalopathy syndrome
Megalencephalic leukoencephalopathy with subcortical cysts. It can also refer to gene MLC1 or Megalencephalic leukoencephalopathy with subcortical cysts 1, a human gene related to the former disease.
Hypertensive leukoencephalopathy

The classification of leukoencephalopathies is a matter of debate. Some authors divide leukoencephalopathies into hereditary disorders and acquired disorders. The hereditary demyelinating disorders are then classified according to the localization of the underlying metabolic defect, and they include the leukodystrophies when myelin growth is the underlying problem.

The acquired demyelinating disorders are classified according to their underlying causes into five groups: noninfectious–inflammatory, infectious–inflammatory, toxic–metabolic, hypoxic–ischemic (vascular problems like Binswanger's disease), and traumatic.

This classification is diffuse sometimes. For example CADASIL is at the same time hereditary and hypoxic.