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13 线粒体疾病 mitochondrial diseases

13 线粒体疾病 mitochondrial diseases. Mutations (changes) in the mitochondrial chromosome are responsible for a number of disorders.

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13 线粒体疾病 mitochondrial diseases

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  1. 13 线粒体疾病mitochondrial diseases

  2. Mutations (changes) in the mitochondrial chromosome are responsible for a number of disorders.

  3. Mitochondrial disease is a chronic, genetic disorder that occurs when the mitochondria of the cell fails to produce enough energy for cell or organ function.

  4. The incidence about 1:3000-4000 individuals in the US.

  5. Characteristics Unlike nuclear genes, which are inherited from both parents, mitochondrial genes are inherited only from the mother. In mammals, 99.99% of mitochondrial DNA (mtDNA) is inherited from the mother. This is because the sperm carries its mitochondria around a portion of its tail and has only about 100 mitochondria compared to 100,000 in the oocyte.

  6. Threshold effect • % of mutant mtDNAs must be above a threshold to produce clinical manifestations • % of mutant mtDNAs needed to cause cell dysfunction varies according to tissue oxidative requirements • Disease signs especially manifest in • Tissues with a high energy expenditure: Dependent on oxidative metabolism • Specific tissues: Brain, Heart & Muscle

  7. Mitotic segregation • % of mutant mtDNAs in daughter cells can shift at cell division • Produces rapid changes of genotype that may lead to crossing of threshold

  8. There are many forms of mitochondrial disease. Mitochondrial disease presents very differently from individual to individual.

  9. Mitochondrial disease is inherited in a number of different ways. There may be one individual in a family or many individuals affected over a number of generations.

  10. If there is a mutation in a mitochondrial gene, it is passed from a mother to all of her children; sons will not pass it on, but daughters will pass it on to all of their children, and so on.

  11. 3. LHON LHON = Leber's; Hereditary; Optic; Neuropathy

  12. Genetic-Clinical correlations: Maternal Inheritance • Recurrence risks: Brother 30%; Sister 8%; Nephew 46%; Niece 10%; Male cousin 31%; Female cousin 6% • 40% of patients with commonest mutation (G11778A) have negative family history • Large families with maternal inheritance: G11778 & T14484C mutations

  13. Mutations (General) • 3 Mutations account for 96% of cases • All in Complex I genes • Mutations: G11778A (69%), G3460A (13%), T14484C (14%)

  14. Clinical features (General) Male predominance:No relation to any X-linked genes Onset :Midlife: Mean 30 years; Range 1 to 70 Visual loss • Clinical features • Painless • Visual loss pattern • Severity: May deteriorate to 20/200 or less • Progression: Mean 4 months; • Interval between eyes affected: ~ 2 months • Tendency to recover depends on mutation • Pupillary reactions: May be relatively spared for degree of visual loss • Ocular pathology Other features: Some families Cardiac conduction defects; Spastic dystonia; Spastic paraparesis; Dystonia

  15. Laboratory • Muscle pathology • No ragged red fibers • EOM mitochondria: Diffuse increase in number and size; Disorganized cristae • Preservation of myofibrils • MRI: Optic nerve may enhance on T2 weighted images

  16. 4. MERRF MERRF=Myoclonic Epilepsy; Ragged Red Fibers

  17. mtDNA point mutations: • tRNA Lys : A8344G (Frequent); T8356C; G8363A; G8361A • Syndromes: MERRF or MERRF/MELAS overlap • tRNA Ser • Syndromes: MERRF/MELAS overlap; Epilepsia Partialis Continua; • tRNA Leu

  18. Onset Late adolescence - Early adult

  19. Clinical syndrome: • CNS • Myoclonus (60%) • Epilepsy (45%) • Cerebellar dysfunction: Ataxia • Dementia • Optic atrophy (20%) • Polyneuropathy (20%) • Distal sensory loss (large fiber modalities) • Hearing loss (40%) • Myopathy • Short stature (10%) • Lipomata (10%)

  20. Laboratory • Lactic acidosis: Variable • Pathology of muscle • Ragged red fibers

  21. 5. MELAS MELAS=Mitochondrial Encephalomyopathy; Lactic Acidosis; Stroke

  22. mtDNA point mutations • tRNA Leu (common) • A3243G mutation: 80% of MELAS syndromes • Other MELAS mutation loci: T3271C has later age of onset; 3291

  23. Clinical Syndrome • Onset • Mean = 10 years; Range = 2 to 40 • Encephalopathy: Often episodic • Systemic features • Myopathy • Polyneuropathy • More common in patients with myopathy • Mean life span with full clinical syndrome ~ 2 to 4 decades

  24. Scattered "ragged red" muscle fibers: Gomori trichrome Scattered abnormal, vacuolated fibers with clear rim: H & E

  25. Ragged red muscle fibers: Gomori trichrome

  26. Genetic counseling: A3423G mutation • % of affected offspring: Increased with higher mutant load in maternal blood • Mutant load 1% to 19%: 20% chance of affected offspring • Mutant load > 20%: 50% chance of affected offspring • Full expression of phenotype in multiple family members: Rare • Partial expression in multiple family members: Common

  27. Laboratory • Lactic acidosis: Blood & CSF • EMG: Mormal or Myopathic • Serum CK: Normal to 2x high (32%) • MRI: Strokes • Biochemistry • Respiratory chain dysfunction • Reduced activity of Complexes I & IV • Pathology (A3243G mutation)

  28. 6. Kearns-Sayre Syndrome Family history • Sporadic: Most patients • Familial cases: Rare; Mother to offspring

  29. mtDNA mutation types • Single large mtDNA deletion (2 to 8 kb) • Most common mutation type (80%) • Common deletions • Most common: 4977 base pairs from 8488 to 13460; 13 base pair repeat at mutation break point • Thai patients: 3558 bp deletion; 10204 to 13761, or 10208 to 13765 • Most deletions preserve • Promoters of transcription of heavy & light strands • 12S & 16S ribosomal RNA genes • Origin of heavy strand replication • Change in number of deletions over time • Increased in muscle • Reduced in rapidly turning over cells (hematopoetic) • Large scale tandem duplication

  30. Clinical features • General • Characteristic signs: PEO; Pigmentary degeneration of retina; Heart block; Mitochondrial myopathy • Onset: < 20 years; Later onset patients may have only PEO • Ocular • External Ophthalmoplegia • Dysphagia: 50% of adults symptomatic • Myopathy • Weakness (90%): Proximal > Distal; Symmetric • Occasional fatigue or pain on exertion • CNS • Hearing loss (95%) • Ataxia (90%) • Systemic features

  31. Laboratory • Muscle pathology • Ragged red fibers (98%): COX + and COX - • Variation in muscle fiber size • Lactic acidosis (80%) • Head CT: Basal ganglia calcifications (5%) • CSF Protein: High

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