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Kearns-Sayre Syndrome

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Presentation on theme: "Kearns-Sayre Syndrome"— Presentation transcript:

1

2 Kearns-Sayre Syndrome
Mohsen Javadzadeh Child Neurologist

3 Background Kearns-Sayre syndrome (KSS) is characterized by the onset of Ophthalmoparesis and Pigmentary Retinopathy before age 20 years. Other frequently associated clinical features include Cerebellar Ataxia Cardiac Conduction Block Raised CSF Protein Content, and Proximal Myopathy.

4 Other findings Short Stature Multiple Endocrinopathies
Diabetes Mellitus Hypoparathyroidism Addison Disease Renal Tubular Acidosis (proximal or distal) with occasional progression to end-stage renal failure Bilateral sensorineural hearing loss almost universal in those who survive into the fourth decade of life; not fully corrected with hearing aids.

5 Pathophysiology The mitochondrial genome is a base-pair closed circular loop of double-stranded DNA found in multiple copies within the mitochondrial matrix It encodes the genetic information for the 13 polypeptide subunits essential for the process of oxidative phosphorylation In addition it encodes 2 ribosomal RNA (rRNA) genes and 22 transfer RNA (tRNA) genes necessary for the intramitochondrial synthesis of these 13 polypeptides

6 The “Cambridge Sequence”
The genome was first sequenced in its entirety in 1981, and this "Cambridge Sequence" was subject to minor revisions in 1999. Mitochondrial DNA (mtDNA) is inherited almost exclusively through the maternal lineage, with only a single report of paternal inheritance. Discriminate the “mitichondrial inheritance” from “mitochondrial disorders”!

7 Heteroplasmy Located within the mitochondrial matrix, and lacking the efficient repair mechanisms available to nuclear DNA, mtDNA has a relatively high rate of mutation. Most of these mutations are inconsequential; however, a stable, replicative mutant mtDNA is sometimes produced. This is not necessarily a problem for the cell or tissue because multiple copies of mtDNA are present in each cell (in oocytes, this is in the region of 100,000 copies per cell), and both wild type and mutated mtDNA can coexist, a situation known as heteroplasmy.

8 Heteroplasmy

9 The Threshold Level Disease only ensues when the proportion of mutated to wild-type mtDNA exceeds a tissue-specific threshold. This is usually in excess of 65% mutated mtDNA but can widely vary between tissues and individuals. Thus, the level of mutant heteroplasmy is an important determinant of the clinical presentation of mitochondrial disease.

10 Mode of Inheritance Kearns Sayre Syndrome (OMIM #530000) occurs as a result of large-scale single deletions (or rearrangements) of mtDNA, which are usually not inherited but occur spontaneously, probably at the germ-cell level or very early in embryonic development. The risk of maternal transmission has been estimated to be approximately 1 in 24(almost 4%).  The deletions vary in size and, although a common deletion of 4.9kB is present in at least a third of patients.

11 Polycistronic Transcription
How can a heterogeneous group of mitochondrial deletions lead to a similar phenotype? The proposed mechanism is based on the knowledge that transcription of mtDNA is polycistronic. It means that all genes encoded on the heavy and light strands are transcribed as 2 large precursor RNA strands. A deletion anywhere in the mitochondrial genome may affect transcription or translation of genes that originally were not affected by the deletion.

12 The Tissue Site Of Deletion
An identical deletion has been identified in patients with 2 other conditions: Pearson syndrome, which is a sideroblastic anemia of childhood, pancytopenia, and exocrine pancreatic failure, and Chronic progressive external ophthalmoplegia (CPEO), which consists of external ophthalmoplegia, bilateral ptosis, and proximal myopathy. Mitochondrial deletions in CPEO tend to be localized in muscle tissue; in Pearson syndrome, mutations occur in hematopoietic cells, explaining the different clinical phenotypes.

13 The “Tangencies” Neither size nor location of the deletion alone determines clinical phenotype. Instead, the phenotype appears to be determined by the relative amounts of deleted and wild-type mtDNA. Very high levels of deleted mtDNA in all tissues are likely to cause Pearson syndrome, in which the dominant feature is pancytopenia. Lower levels of deleted mtDNA cause Kearns-Sayre syndrome. In CPEO, deleted mtDNA may be detected only in muscle tissue. CPEO and Kearns-Sayre syndrome vary in the location and percentage of mtDNA deletion. Exceptions are recognized, and survivors of the pancytopenic crisis of Pearson syndrome can also develop Kearns-Sayre syndrome.

14 The Tangencies

15 Epidemiology Frequency Mortality/Morbidity
A rare disorder The prevalence not precisely stated, but estimated to be about 1.1 to 1.6 per adult population. No known racial or sex predilection. Part of its characterization is onset in individuals younger than 20 years. Mortality/Morbidity Although Kearns-Sayre syndrome probably reduces life expectancy, no numerical data are available. Morbidity depends on severity and the number of systems or organs involved, which widely varies from patient to patient. Heart block is a significant and preventable cause of mortality.

16 Presentation Muscle weakness
Chronic and progressive decreased eye movements and ptosis Dysphagia Skeletal muscle weakness (proximal more than distal) and exercise intolerance CNS dysfunction Ataxia Dementia, encephalopathy, or specific focal neuropsychological deficits Deafness Night blindness

17 Pigmentary Retinopathy

18 Heart Block

19 Ptosis

20 Other Organs Cardiac disease Symptoms of endocrine dysfunction Syncope
Palpitations Symptoms of endocrine dysfunction Diabetes mellitus Menstrual irregularities, delayed puberty Poor growth, failure to thrive Seizures due to hypocalcemia (hypoparathyroidism)

21 Differential Dignoses:
Atrioventricular Block, Third Degree, Acquired Chronic Progressive External Ophthalmoplegia Failure to Thrive MELAS Syndrome Myasthenia Gravis Pearson Syndrome Retinitis Pigmentosa

22 Laboratory Studies Blood lactate and pyruvate. CSF lactate levels are elevated even if blood lactate levels are within the reference range. CSF protein levels are very frequently elevated. Serum creatinine kinase Single large-scale deletions may be detectable in blood. Or, diagnosis may be established by muscle biopsy with histochemistry and mtDNA analysis for major rearrangements. Screening to exclude the endocrinologic abnormalities is recommended in many patients. Measure serum electrolyte, glucose, calcium, magnesium, and plasma cortisol levels as well as thyroid function. Urine measurements of pH, protein, glucose, and amino acid

23 Imaging Studies MRI of the brain may reveal subcortical white matter lesions (hyperintense on T2 and FLAIR) along with involvement of thalamus, basal ganglia, and brainstem. Cerebral and cerebellar atrophy may be present.

24   Other Tests ECG reveals cardiac conduction defects; measurement of the PR interval is indicated. Echocardiography is used to look for cardiomyopathy. Electroretinography helps assess retinal degeneration. Audiometry helps detect sensorineural deafness. Electroencephalography during period of encephalopathy reveals generalized slow wave activity. Electromyography and nerve conduction findings may be normal or may show mild myopathy with or without neuropathy. 

25 Procedures Perform a lumbar puncture and measure protein and lactate levels in the CSF. Muscle biopsy may reveal ragged red fibers. Muscle histochemistry reveals deficiency of cytochrome c oxidase.

26 Histological Findings
As with other mitochondrial encephalopathies, spongy degenerative changes occur in both the gray and white matter of the brain. Gray matter loss is also seen in the brainstem and Purkinje cell layer. Calcium deposits accumulate in the globus pallidus and thalamus. Large mitochondria with abnormal structure develop in both skeletal and heart muscles.

27 Large, abnormal mitochondria

28 Medical Care & Consultations
No disease-modifying therapy is available for KSS. Management is supportive vigilance for detection of associated problems. All patients with KSS require consultation with an ophthalmologist, a cardiologist, endocrinologist, and psychologist. Genetic counseling is also indicated. Supplementation with coenzyme Q10 and folinic acid may be indicated. Exercise may help patients with myopathy.

29 Thanks For Your Atention

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