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PMY2106 > Angiogenesis 2 > Flashcards

Angiogenesis 2 Flashcards

1
Q

anti-angiogenic therapy

A

“does not aim to destroy tumours, but instead by limiting their blood supply it attempts to shrink tumours and prevent them from growing”

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2
Q

5 classes of angiogenic antagonists

A
  • inhibitors of proteases
  • inhibitors of endothelial cell migration and proliferation
  • inhibitors of angiogenic growth factor
  • inhibitors of matrix proteins on endothelial cell surface, such as integrins and copper
  • inhibitors with unique mechanisms
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3
Q

anti-VEGF therapies

A
  • monoclonal antibodies directed against specific proangiogenic growth factors or their receptors
  • small molecule tyrosine kinase inhibitors of multiple proangiogenic growth factor receptors
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4
Q

bevacizumab

A

monoclonal antibody against VEGF-A

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5
Q

ramucirumab

A

monoclonal antibody to VEGFR-2

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6
Q

monoclonal antibody to VEGFR-2

A

tyrosine kinase inhibitors that target VEGF receptors

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7
Q

process of VEGF binding

A

VEGF binds to receptor -> receptor dimerisation and autophosphorylation -> production of various proangiogenic factors

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8
Q

ANTI-VEGF

A
  • bevacizumab
  • recombinant anti-VEGF MAb
  • T 1/2 = 14-21 days
  • neutralises all forms of VEGF
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9
Q

Side effects of bevacizumab

A
  • hypertension
  • proteinuria
  • gi perforations
  • bleeding
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10
Q

alfibercept

A
  • protein comprised of segments of the extracellular domains of VEGFR1 and VEGFR2
  • fused to constant region (Fc) of human IgG1
  • functions as soluble decoy receptor, binds VEGF and prevents it binding to actual VEGF receptor
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11
Q

protein kinases

A
  • catalyse transfer of gamma phosphate from ATP to one of more amino acid residues in a protein substrate side chain
  • results in conformational change, affecting protein function
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12
Q

tyrosine kinase inhibitors structure

A
  • ligand binding extracellular domain
  • single transmembrane domain
  • cytosolic tyrosine kinase domain
  • flexible C-terminal tail
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13
Q

how RTK inhibitors work

A
  • phosphorylation sites that promote TKD activation present in juxtamembrane domain, activation loop and C-terminal tail
  • activation loop resides within active site of TKD thus sterically hindering access by ATP to nucleotide-binding pocket
  • phosphorylation of activation loop promotes conformational changes, inducing swinging out of activation loop which releases auto-inhibition effects as well as stabilising activated TKD
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14
Q

NRTKs (non-receptor tyrosine kinases)

A
  • subgroup of tyrosine kinases, intracellular cytoplasmic proteins or anchored to membrane of cell
  • 9 subfamilies according to sequence similarities
  • each NRTK family defined according to sequence homology of kinase domain
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15
Q

how sorafanib works

A
  • inserts into hydrophobic pocket within catalytic loop of RAF-1
  • prevents receptor kinase from binding ATP and phosphorylating their respective tyrosine target residues
  • targets ATP binding domain and competes with ATP
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16
Q

sorafanib issues

A
  • potency of sorafenib becomes lower and lower due to resistance development
  • extremely expensive
17
Q

thalidomide

A
  • was originally marketed as a sedative
  • since tissues are most sensitive to thalidomide when undergoing growth, extreme birth defects in pregnant women taking thalidomide
  • thalidomide inhibits angiogenesis at that stage
  • apoptogenic for neovasculature
18
Q

how thalidomide works

A
  • binds to cereblon, a ubiquitin ligase
  • degrades numerous targets, mostly zinc finger-containing transcription factors
  • efficaciously inhibits pro-angiogenic factors
19
Q

factors thalidomide inhibits

A

factors thalidomide inhibits

20
Q

limitations of anti-angiogenic therapy

A
  • cannot irradiate tumours as a stand-alone strategy
  • prolonged administration reduces microvascular density within tumours, compromising delivery of chemo to tumour cells
  • is a very complex process involving many growth factors and cellular processes
21
Q

hallmarks of resistance to antiangiogenic therapy

A
  • growth factor redundancy
  • recruitment of bone marrow-derived cells
  • local stromal cells
  • vessel co-option and vasculogenic mimicry
  • increased metastasis
  • other emerging mechanisms
22
Q
  • growth factor redundancy
  • recruitment of bone marrow-derived cells
  • local stromal cells
  • vessel co-option and vasculogenic mimicry
  • increased metastasis
  • other emerging mechanisms
A
  • macugen
  • ranibizumab
  • bevacizumab
  • aflibercept
23
Q

how do anti-VEGF therapies treat diabetic retinopathy and macular degeneration

A
  • drug injected into vitreous of the eye and passes into sub retinal space where vessels proliferate
  • neovascularization is then blocked, preventing bleeding into retina
24
Q

do all drugs require intravitreal injection?

A

no

PMY2106 (15 decks)

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