1-47 Correcting Protein Defects Flashcards
the protein only hypothesis
it explains prion diseases (amyloid diseases)
describe the protein only hypotehsis
Prion proteins (PrP) interchange between
PrPc - nonpathogenic, soluble, protease sensitive,mainly alpha helix
PrPsc - pathogenic, insoluble, protease insensitive, and 50/50 alpha helix beta sheet.
when PrPsc proteins come together, they bind together via beta sheet interactions that are very stable. this prevents them from chaging back into the PrPc form and also creates a nucleus which other PrPsc proteins rapidly bind
pore hypothesis
supported by Islet amyloid polypeptide IAPP
posits that still developing soluble oligomers are more toxic than the mature fibrils in amyloid disease
as oligomers are growing, they diffuse into the cell membrane and form a pore to disrupt it
once a large enough beta confirmation fibril is formed, will bud off back into cytosol
according to pore hypothesis, what happens when we introduce mature fibrils into affected cells?
could be protective - the IAPP proteins would aggregate with the fibrils (the template) in the cytosol instead of disrupting the cell membrane
receptor hypothesis
supported by ab42
suggests that prion oligomers bind receptors and alters signal pathways
specifically, binding glutamate receptor in alzheimers and creutzfeldt disease.
studies preventing abeta42 and PrPc from binding the glutamate receptor in mice has been promising
how does a defect or mutation affects properties of the protein and how this gives rise to disease symptoms
in prion diseases - beleived that normal PrP’s experience mutation that causes equilibrium to shift toward the PrPsc more than normal
this increases the likeliehood of a beta structure nucleation event
what effect does the apolipoprotein E taking on the isoform ApoE4 have?
salt bridge formation between arg and glu residue causes preferential binding to VLDL and a-beta.
people with this isoform have greater risk of cardiovascular disase (due to VLDL bidning) and alzhiemers disease (a-beta binding)
describe transthyretin amyloidosis
TTR protein that binds/transports thyroxine is mutated into form that can form amyloid fibrils
TTR is in equilibrium between two states - a tetramer and monomer
monomer forms amyloid
mutations that push equilibrium towards the monomer form cause the disease which spreads around the body causing mutliple organ failure
amyloid cascade hypothesis vs other hypotheses that describe how “toxic folds” kill cells and cause disease
amyloid cascade - it is the mature fibrils that lead to cell death in amyloid diseases
other hypotheses maintain taht the formation of amyloids is a side effect of teh disease, and that soluble oligomers are what cause symtpoms
what would be a viable strategy of lowering alzheimers risk?
disruption of the inter-residual salt bridges of ApoE4
what would be a viable strategy to combat TTR amyloidosis
small drugs have been designed to bind TTR’s thyroxine binding site and stabalize the tetrameric form.
goal is to stabalize enough tetramer while still leaving thyroxine binding sites open
Alpha-1-antitrypsin is a good example because..
its a serine protease and is an example of a disease due to misfolding that can result from either aggregation or lack of function
describe the RCL loop and neutrophil elastase
NE sees the reactive center loop, bites it, forms covalent bond
loop cleaved and now is intserted into central beta sheet (has complemetnary sequences)
-it drags neutrophil elastase down to lower section of alpha 1
the interaction of alpha 1at and neutrophil elastase causes it to unfold (destabalizes it), which allows other proteases to come and degrade it
two things that can go wrong with alpha-1-antitrypsin
- when RCL inserts into beta sheet, it is sprung by itself. more stable, can’t go back and can’t inhibit anymore. If this happens enough due to mutation, can no longer inhibit neutrophil elastace which proceeds to chew up things it shouldnt
- if insertion occurs without cleavage, and it mis-inserts into a neighbor molecule causing a stabalizing aggregating chain reaction. Can occur in liver where concentration is high. Builds up and causes liver failure
the isomutation of alpha-1-antitrypsin causes..
destabaliziation of the beta sheet
