Download Comment in GO: This term is intended to

Neurofibrillary Tangles and
Amyloid Plaques:
The Treatment of Protein Aggregates in the
Protein Ontology
Alexander P. Cox and Alexander D. Diehl
University at Buffalo (SUNY)
Protein Ontology Workshop
Georgetown University June 18-19, 2014
Existing Terminology in GO & PRO
macromolecular complex (GO:0032991)
– A stable assembly of two or more macromolecules, i.e. proteins, nucleic
acids, carbohydrates or lipids, in which the constituent parts function
together.
protein complex (GO:0043234)
– Any macromolecular complex composed of two or more polypeptide
subunits, which may or may not be identical. Protein complexes may have
other associated non-protein prosthetic groups, such as nucleotides,
metal ions or carbohydrate groups.
 Comment in GO: This term is intended to exclude structures composed of the
same repeating subunit or subunits, for example microtubules. Protein
complexes encompassed by this term are generally not structural, and usually
have a defined set of subunits.
Existing Terminology in GO & PRO
macromolecular complex (GO:0032991)
– A stable assembly of two or more macromolecules, i.e. proteins, nucleic
acids, carbohydrates or lipids, in which the constituent parts function
together.
protein complex (GO:0043234)
– Any macromolecular complex composed of two or more polypeptide
subunits, which may or may not be identical. Protein complexes may have
other associated non-protein prosthetic groups, such as nucleotides,
metal ions or carbohydrate groups.
 Comment in GO: This term is intended to exclude structures composed of the
same repeating subunit or subunits, for example microtubules. Protein
complexes encompassed by this term are generally not structural, and usually
have a defined set of subunits.
What is a Protein Aggregate?
Common Conceptions
– Necessarily composed of misfolded proteins
– Necessarily disorganized
– Necessarily non-soluble
– Necessarily pathological or indicative of pathology
What is a Protein Aggregate?
Common Misconceptions
– Necessarily composed of misfolded proteins
• Not always – immune complexes are protein aggregates
– Necessarily disorganized
• Not always – prions polymerize in a regular, efficient way
– Necessarily non-soluble
• Not always – solubility is a secondary characteristic of protein aggregates that
depends on size, hydrophobicity, etc.
– Necessarily pathological or indicative of pathology
• Not always – immune complexes and the formation of fibrin aggregates in
coagulation are normal physiological responses
Representing Protein Aggregates
BFO:object aggregate
macromolecule aggregate
protein aggregate
amyloid plaque
has part
has part
has part
ChEBI:macromolecule
PR:amino acid chain
PR:amyloid beta 42 peptide
Macromolecule Aggregate
Working definition:
An object aggregate whose primary constituents are two or more
macromolecules assembled in varying configurations from instance
to instance. A macromolecule aggregate may contain secondary
constituents such as small molecules or ions.
– Elucidation 1: A primary constituent is a constituent that compromises the
majority of the mass of the aggregate.
– Elucidation 2: A varying configuration includes the possibility of varying the
amount of the primary constituent as well as the way the primary constituent is
assembled within an instance of a macromolecule aggregate.
Protein Aggregate
Working definition:
A macromolecule aggregate whose primary constituents are
proteins assembled in varying configurations from instance to
instance.
– Elucidation 1: Proteins compromise the majority of the mass of the aggregate.
– Elucidation 2: A varying configuration includes the possibility of varying the
amount of the individual proteins as well as the way these proteins are assembled
within an instance of a protein aggregate.
Types of Protein Aggregates
– Semi-disordered aggregations of normally folded proteins
– Disordered aggregations of misfolded proteins
– Protein polymers or oligomers assembled in a regular structure
– Fibril aggregates
Types of Protein Aggregates
– Semi-disordered aggregations of normally folded proteins
• immune complexes
• activated proteins of the clotting cascade
• aggregates of foreign protein, typically left after virus replication
– Disordered aggregations of misfolded proteins
• misfolded proteins in endoplasmic reticulum or cytoplasm
• some inclusion bodies (e.g. IPODs, JUNQs, aggresomes)
– Protein polymers or oligomers assembled in a regular structure
• microtubules
• polymerized prions
• myosin fibers
– Fibril aggregates
• amyloids (e.g. amyloid plaques, Lewy bodies)
• neurofibrillary tangles
Immune Complexes
Proposed definition: An immune complex is a protein aggregate
comprised of a network of immunoglobulins bound to epitopes on
cognate antigens. An immune complex may include immunoglubulins
of varying affinity and isotype.
Image From: http://www2.estrellamountain.edu/faculty/farabee/biobk/biobookimmun.html
Aggregates of Misfolded Proteins
http://cardiovascres.oxfordjournals.org/content/85/2/253/F1.expansion
IPODs & JUNQs
Wikipedia: IPOD and JUNQ
Prions
Wikipedia: Prion
Amyloids
– Insoluble fibrous protein aggregates with a beta sheet structure
– Typically extracellular
– Can be composed of various proteins (e.g. amyloid beta, alphasynuclein, huntingtin, ubiquitin) and typically contain serum
amyloid P-component
– Typically, though not always, associated with pathology
• melanosomes are nonpathological amyloids composed of the
Pmel17 protein
Diseases Featuring Amyloids
Wikipedia: Amyloid
Protein Aggregates & Associated Diseases
Aggregate
Disease
amyloid
amyloidosis
amyloid plaque
Alzheimers disease
neurofibrillary tangle
Alzheimers disease
Lewy body
Parkinsons disease; Lewy body dementia
polymerized prions
prion disease (e.g. Creutzfeldt-Jacob disease)
Rosenthal fiber
Alexander disease
Mallory body
Wilsons disease; alcoholic liver disease
intraneuronal ubiquitin inclusion
motor neuron disease
intranuclear Huntingtin inclusion
Huntingtons disease
Bunina body
amyotropic lateral sclerosis
Pick body
Pick’s disease
glial cytoplasmic inclusion
multiple system atrophy
misfolded beta-hexosaminidase
Tay-Sachs disease
straight filaments
progressive supranuclear palsy
The Neurological Disease Ontology (ND)
– Extends the Ontology for General Medical Science (OGMS) to
represent diseases that affect the human nervous system
– Contains approximately 200 subclasses of ‘neurological disease’
classified based on the primary disease mechanism
– Provides a comprehensive representation of neurological diseases
that includes the disease, disease course, syndrome, disorder,
signs and symptoms, diagnosis, diagnostic guideline, and
material/genetic basis
When is Protein Aggregation Pathological?
In general, a biological process can be pathological because:
– Whenever present, it is always leads to a disorder
– It occurs too frequently
– It occurs too infrequently
– Alternatively, process A can be said to become pathological when
another process B slows down or stops such that the effects of
process A then becomes toxic
• For example, amyloid aggregation may become pathological only
when amyloid aggregate clearance stops working properly and allows
the buildup of dangerous levels of amyloid plaques.
Tangles, Plaques, & Lewy Bodies
Neurofibrillary tangles
– Composed primarily of hyperphosphorylated tau
– Associated with Alzheimer’s disease and frontotemporal dementia
Amyloid plaques
– Composed primarily of amyloid beta
– Associated with Alzheimer’s disease
Lewy bodies
– Composed primarily of alpha-synuclein and ubiquitin
– Associated with Lewy body disease and Parkinson’s disease
Aggregates
BFO: object
aggregate
protein
aggregate
Lewy body
amyloid
aggregate
macromolecule
aggregate
neurofibrillary
tangle
amyloid
plaque
Amyloid Plaques & Neurofibrillary Tangles
Amyloid Plaques & Neurofibrillary Tangles
http://www.nature.com/nrn/journal/v9/n7/box/nrn2420_BX1.html
Representing Causal Hypotheses in ND
• testable hypothesis (OBI_0001908)
– An information content entity that expresses an assertion that is
intended to be tested.
• Alzheimers disease neurofibrillary tangle hypothesis
– The testable hypothesis that the degree of dementia resulting from
Alzheimers disease more directly correlates with the formation of
neurofibrillary tangles than amyloid plaques in the brain.
• Alzheimers disease amyloid cascade hypothesis
– The testable hypothesis that Alzheimers disease is caused, at least in
part, by the accumulation of amyloid plaques in the cortex, hippocampus,
basal forebrain, or brain stem regions of the brain.
Neurofibrillary Tangle Hypothesis
http://www.nature.com/nm/journal/v11/n8/fig_tab/nm0805-826_F1.html
Amyloid Cascade Hypothesis
Biochemical Society Transactions (2005) 33, 553-558 - www.biochemsoctrans.org
Aggregates
BFO: object
aggregate
protein
aggregate
Lewy body
amyloid
aggregate
macromolecule
aggregate
neurofibrillary
tangle
amyloid
plaque
Proteins & Aggregates
BFO: object
aggregate
protein
aggregate
amyloid
plaque
Lewy body
amyloid
aggregate
CHEBI: macromolecule
has part
has part
has part
has part
has part
neurofibrillary
tangle
macromolecule
aggregate
PR: tau
PR: amyloid-beta 42
PR: amyloid
PR: amino
acid chain
PR: protein
PR: ubiquitin
PR: alpha-synuclein
has part
Aggregates & Diseases
BFO: disposition
ND: Lewy body
disease
ND: amyloidosis
linked to
ND: frontotemporal
ND: Alzheimers
dementia with
disease
Parkinsonism
ND: tauopathy
BFO: object
aggregate
linked to
OGMS: disease
protein
aggregate
amyloid
aggregate
Lewy body
linked to
macromolecule
aggregate
neurofibril ary
tangle
amyloid
plaque
linked to
Aggregates, Processes, & Diseases
BFO: object
ag regate
macromolecule
ag regate
protein
ag regate
produces
GO: biol gical
proces
BFO: proces
has part
OGMS: disease
course
protein GO: protein ND: amyloidosi ND: tauopathy
ag regation polymerization disease course disease course
has particpant
has particpant
has part has part
tau ag regation
has particpant
has particpant
has part
realizes
realizes
realizes
realizes
realizes
realizes
BFO: dispositon
OGMS: disease
ND: tauopathy ND: amyloidosi
ND: fronto emporal
ND: fronto emporal
ND: Alzheimers ND: Lewy body
neurofibrilary amyloid amyloid plaque GO: amyloid ND: Lewy body ND: Alzheimers dementia with
dementia with
disease disease
tangle ag regate formation fibril formation disease course disease course Parkinsonism
Parkinsonism
disease course
produces
amyloid
Lewy body
plaque
produces
Aggregates & Processes
BFO: object
aggregate
protein
aggregate
amyloid
aggregate
macromolecule
aggregate
neurofibril ary
tangle
produces
GO: biological
process
BFO: process
has part
has participant
has participant
OGMS: disease
course
protein GO: protein ND: amyloidosis ND: tauopathy
aggregation polymerization disease course disease course
has part
tau aggregation
has participant
has participant
has part
has part
ND: frontotemporal
amyloid plaque GO: amyloid ND: Lewy body ND: Alzheimers dementia with
formation fibril formation disease course disease course Parkinsonism
disease course
produces
amyloid
Lewy body
plaque
produces
Proteins, Aggregates, & Processes
CHEBI: macromolecule
BFO: object
ag regate
protein
ag regate
macromolecule
ag regate
has part
has participant
P R : a mi n o
acid chain
PR: protein
has part
has part
has participant
amyloid
has part plaque
has part
produces
produces
produces
Lewy body
GO: biological
proces
BFO: proces
has part
OGMS: disease
course
protein GO: protein ND: amyloidosis ND: tauopathy
ag regation polymerization disease course disease course
has participant
has participant
has part has part
tau ag regation
has participant
has participant
has part
ND: frontotemporal
PR: tau
neurofibril ary amyloid amyloid plaque GO: amyloid ND: Lewy body ND: Alzheimers dementia with
tangle ag regate formation fibril formation disease course disease course Parkinsonism
disease course
PR: amyloid
PR: ubiquit n PR: amyloid-beta 42
PR: alpha-synuclein
has part
has participant
Proteins, Aggregates, Processes, & Diseases
CHEBI:macromolecule
P R : a m in o
acidchain
PR:protein
haspart
haspart
hasparticpant
haspart
BFO:object
ag regate
macromolecule
ag regate
protein
ag regate
hasparticpant
amyloid
produces
produces
GO:biol gical
proces
BFO:proces
haspart
OGMS:disease
c ou r s e
protein GO:protein ND:amyloidosi ND:tauopathy
ag regation polymerization diseasecourse diseasecourse
hasparticpant
hasparticpant
haspart haspart
tauag regation
hasparticpant
haspart
realizes
realizes
realizes
realizes
realizes
realizes
BFO:dispositon
OGMS:disease
ND:tauopathy ND:amyloidosi
ND:frontoemporal
PR:tau
ND:frontoemporal
neurofibrlary amyloid amyloidplaque GO:amyloid ND:Lewybody ND:Alzheimers dementiawith ND:Alzheimers ND:Lewybody
dementiawith
tangle ag regate formation fibrlformation diseasecourse diseasecourse Parkinsonism disease disease
Parkinsonism
diseasecourse
PR:amyloid
PR:ubiquitn PR:amyloid-beta42
haspart
produces
L e w y bo d y
PR:alpha-synuclein
hasparticpant
haspart plaque
haspart
hasparticpant
Discussion: Linking Proteins to Diseases
• ND’s asserted hierarchy groups neurological diseases based on the primary
mechanism. In many cases, this is thought to be protein
misfolding/aggregation (e.g. amyloidosis, tauopathy, alpha-synucleinopathy).
Thus, ND already asserts a connection between certain diseases and proteins.
• Is ‘OGMS: has material basis’ a shortcut relation between diseases and
proteins? Is this what we want? Is it too strong or too weak?
• Asserting protein participation in a disease course or pathological process is
not an assertion of causality. Does this make participation too weak?
• Do we need an explicitly causal relation? If so, what and how do we define it?
Future Work
• Finalize definitions for key terms and move relevant terms to PRO
and GO
• Add enhanced representations for additional protein aggregates
• Represent additional disease courses and causal disease
hypotheses involving protein aggregates
• Identify additional methods for linking proteins and diseases
• Refine the distinction between pathological and non-pathological
protein aggregates
Acknowledgments
PRO Consortium
Mark Jensen
Patrick L. Ray
Travis Allen
Alan Ruttenberg
Barry Smith
Alexander D. Diehl
Thanks to PRO Grant NIGMS 2R01GM080646-06 for project funding!
ND publications and OWL file:
https://code.google.com/p/neurological-disease-ontology/
Contact us:
Alexander P. Cox - [email protected]
Alexander D. Diehl - [email protected] (PI)