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Transcript
Mitochondrial dysfunction
• Monogenic mitochondrial disorders
• Pathologic conditions such as:
– Alzheimer’s disease
– Parkinson’s disease
– Huntington’s disease
– cancer
– diabetes
– obesity
– epilepsy
– cardiac disease
• Progressive decline in the expression of mitochondrial genes is a central
feature of normal human aging
– It is not entirely clear whether these changes in expression have positive of negative
effect on life span
Mitochondrial dysfunction – additional
sources
• off target effects of environmental toxins (e.g. rotenon)
• frequently used drugs (e.g. statins, amiodarone , antipsychotic drugs,
valproic acid-epilepsy, zidovudine- HIV treatment)
• antibiotics
• aspirin
• chemotherapeutic agents (e.g. doxorubicin)
Monogenic mitochondrial diseases
Monogenic mitochondrial diseases has considerably advanced
our understanding of the cellular pathophysiology of
mitochondrial dysfunction
This review summarizes these insights and explain how they can
contribute to the rational design of intervention strategies for
mitochondrial dysfunction
Structure
• Mitochondrial internal and external structure varies with
– cell type
– metabolic state
– and often becomes altered during mitochondrial dysfunction
Mutation in
NDUFS2 –
Complex I
Structure
The inner membrane contains many matrix- protruding folds (cristae)
that increase the surface area of the inner membrane and have a
dynamic structure.
These structural dynamics may serve to regulate mitochondrial
metabolism
Function
Best known – production of ATP
But also metabolite exchange, ion transport, protein import, production of
reactive oxygen species, apoptosis
Monogenic cell models of mitochondrial
dysfunction
With the use of mitochondrial proteome analysis ~1000 genes encoding mitochondrial proteins were discovered
in humans (Pagliarini, Cell 2008)
Mitochondrial dusfunction can arise from a mutation in one of
these genes – primary mitochondrial disorder
or from an outside influence on mitochondria - secondary
mitochondrial disorder (e.g. drugs)
Mutations in 228 protein-encoding nDNA genes and 13 mtDNA genes
have been linked to a human disorder
Cancer of colon,
Alzheimer’s disease,
Complex I deficiency
Renal cell
cancer
Diabetes
Epilepsy
Mutations and phenotypes
• It is not clear how specific genetic defects are linked to dysfunction at the
level of cells, organs, and the whole organism
• It is difficult to determine the effects of specific defects because of
compensatory stress–response pathways:
–
–
–
–
–
Mitochondrial biogenesis
Increased expression of oxidative phosphorylation proteins
A switch to a more glycolytic mode of ATP production
Removal of dysfunctional mitochondria by quality-control systems
The substrate supply, the mode of ATP generation, the level of demand
for ATP, mitochondrial dynamics, rate of oxidative phosphorylation
differ among cell types and tissue types
cellular level
Various types of tissues are not equally sensitive to mitochondrial dysfunction
Genetic background also modifies the phenotype of human
mitochondrial diseases. Manifested only when a certain threshold of
Organism level
mitochondrial dysfunction or cellular demand on mitochondrial metabolism is exceeded
Developing a rational intervention strategy
• The functional properties of isolated mitochondria differ considerably
from those within the cell
• Mitochondrial function can also be investigated in intact (patient) cells
Developing a rational intervention strategy
In a primary mitochondrial disorder, the mutation
- affects the expression level of protein, its function, or both
- induces primary cell consequences and secondary cell consequences:
reduced ATP production
increases in the cellular levels of mitochondrial proteins and mitochondrial
function
upregulation of the detoxification of reactive oxygen species
It appears that primary and secondary mitochondrial disorders have similar
consequences at the cellular level
Developing a rational intervention strategy
Four intervention strategies for mitochondrial dysfunction have
been described:
– Genetic therapy- carried out at the preclinical level, mainly on mtDNAassociated disorders (not included in the review)
aim to:
– Small molecules to target mitochondrial dysfunction
1. Increase ATP synthesis
2. Bypass the
– Metabolic manipulation
mitochondrial defect
– Diet and exercise
3. Stimulate
mitochondrial biogenesis
? 4. Reduce levels of ROS
ROS can act as signaling molecules, and therefore, their elimination
might also have detrimental effects
Small molecules
• Specific targeting of mitochondria by small molecules
(referred to as “cargo”) can be achieved by
• Protein-based cargo can be coupled to a mitochondrial targeting sequence
recognized by the mitochondrial protein import machinery
• Coupling the cargo to a delocalized lipophilic cation, leading to its
accumulation in mitochondria
(Several antioxidants have been successfully targeted using the cation
approach such as CoQ variant )
• Mitochondria-penetrating peptides are engineered cell-penetrating
peptides that target mitochondria on the basis of their membrane
potential and lipophilicity
• Vesicle-based transporters that target mitochondria through
macropinocytosis, endosomal escape, and membrane fusion
Intervention strategies for mitochondrial disease
Treatment
•
•
•
•
•
In 2006 – large scale review of published clinical trials of treatments for primary
mitochondrial disorders revealed no evidence supporting the use of any
intervention
Several recent trials in which a variety of treatments for mitochondrial disease
were studied, including dichloroacetate, vitamins, and a cocktail of specific food
components showed a positive effect
CoQ10 variant (idebenone)- was approved for the treatment of Friedreich’s ataxia
(iron)
A ketogenic diet was effective in preventing epileptic seizures in children with
electron-transport-chain defects - suggesting that it may be worthwhile to pursue
nutritional treatment strategies
Ullrich’s congenital muscular dystrophy and Bethlem’s myopathy are associated
with mitochondrial dysfunction and muscle-cell apoptosis (inappropriate opening
of the mitochondrial permeability transition pore) prevented in patients treated
with a permeability transition- pore desensitizer, cyclosporin A
Future perspectives
• A field that began more than 50 years ago, when a physician detected a
mitochondrial disorder in a single patient with hypermetabolism, has now
evolved into the discipline of mitochondrial medicine
• Lessons learned from studies of rare diseases have implications for a
broad range of medical disciplines
• Within the next few years, the application of new technologies (e.g.
whole-exome sequencing) will result in a huge expansion of the number of
known causative nuclear gene defects in patients with mitochondrial
diseases
• The challenge - to increase our understanding of the consequences of
mitochondrial dysfunction at all levels of complexity in order to drive the
development of rational treatment strategies
• Direct enzyme-replacement therapy may be feasible in addressing singleprotein enzymes, such as those in the tricarboxylic acid cycle
Future perspectives
• Given the metabolic individuality in humans, we do not expect
monotherapeutic metabolic manipulation strategies to be a magic bullet
but predict that the next step in treatment development will be the use of
combinations of manipulation strategies applied in an individualized way
• In the meantime, efforts must be made on a global scale to genetically
categorize patient cohorts, monitor them in a standardized way by means
of prognostic scoring systems, and develop new biomarkers to allow for
proper monitoring of the effect of intervention strategies