Signaling Pathways and Development Flashcards
similarities of hedgehog (Hh) and Wnt pathways (3)
regulated by proteolysis
involved in embryonic development
involved in maintaining stem cell niches (implicated in cancer)
contrast developmental roles of
Sonic Hh
Indian Hh
Desert Hh
Sonic Hh: CNS
Indian Hh: cartilage and bone
Desert Hh: peripheral nerves
what are the transcriptional effectors of Hh family genes
Ci (Drosophila) //
Gli1/2/3 (mouse and human)
describe these components of Hh signaling pathway:
a. Hedgehog
b. Patched-1 (Ptc1)
c. Smoothened (Smo)
d. Gli/Ci proteins
e. PKA
a. Hedgehog (Shh, Ihh, Dhh): ligands, secreted hydrophobic proteins produced by localized group of cells (embryos and adults)
b. Patched-1 (Ptc1): 12-TM receptor, binds Hh ligands
c. Smoothened (Smo): 7-TM GPCR (*does NOT bind Hh, is BLOCKED by Ptc1)
d. Gli/Ci proteins: TF that activator or repress target gene expression depending on signaling status
e. PKA: phosphorylates Gli/Ci to target them for proteolysis in proteosome
what happens in Hh pathway when Ptc1 is present as receptor
- Hh ligand binds to Ptc1, preventing it from inhibiting Smo —> Smo is DISinhibited
- Smo disinhibition prevents PKA phosphorylation of Gli proteins
- Smo BLOCKS conversion on Gli proteins into repressors —> Gli proteins are DISinhibited to become activators (GliA) of target genes
what happens in Hh pathway when Ptc1 is NOT present as receptor
- Hh cannot bind Ptc1 —> Ptc1 continues to inhibit Smo
- Gli proteins are phosphorylated by PKA and directed to proteosome
- C-terminus is cleaved —> Gli proteins are converted into transcriptional repressors (GliR) of target genes
how do Shh signaling transduction components localize to the primary cilium (non-motile cilium, sensors of extracellular information)
- Ptc1 inhibits Smo
- Gli proteins shuttled in/out of cilium by IFT (intraflagellar transport proteins)
- Shh ligand binds Ptc1, Smo is disinhibited
- Smo enters cilium and blocks Gli phosphorylation —> GliA
[IFT move cellular cargo in/out of cilia to cell body along microtubules, using kinesin/dynein]
congenital (inherited) human disorders of Hh signaling primarily affect ___ and ____
limb and CNS
Shh is localized to organizing centers in posterior limb bud and ventral midline of CNS during embryogenesis
major biological causes (2) of human holoprosencephaly (HPE)
HPE: failure of embryonic prosencephalic vesicle to divide into two hemispheres
major causes:
1. SHH protein haplo-insufficiency (single copy of gene is not sufficient)
2. GLI2 mutation
[Shh knockout (Shh-/-) in mice induces HPE and limb defects, but limb defects NOT seen in humans]
what is the mechanism and effect of cyclopamine (plant alkaloid)
inhibits Shh signaling by blocking Smo (which Shh disinhibits by binding Ptc1)
Gli phosphorylation into GliR occurs constitutively (target genes constantly repressed)
what is the role of cholesterol in Hh signaling
required for production and secretion of mature Hh protein - needed for self-cleavage reaction that truncates Hh protein precursor
processed form of Hh contains covalent cholesterol adducts in active signaling sequence
Smith-Lemli-Opitz Syndrome
mutation in cholesterol synthesis [sterol delta-7-reductase]
cholesterol depletion during gestation —> depleted processing of Shh (needed for auto-cleavage)
phenotypes similar to knock down of Shh (limbs and CNS effects)
[SHHmith-lemLESTEROL syndrome]
mutations in this component of Hh signaling are linked to related autosomal dominant syndromes with limb and brain defects
[Greig Cephalopolysyndactyly, Pallister-Hall, Postaxial Polydactyly]
GLI3 —> loss of Gli3R (repressing Gli —> GOF mutation in Shh pathway)
what mutation occurs in the Hh pathway in medulloblastoma?
medulloblastoma: tumor in cerebellum during development
Ptc1 mutation (LOF) causes constant disinhibition of Smo, even in absence of Hh ligand (target genes constantly activated)
why is Smo a good drug target and how can it be utilized
Smo is 7-TMR GPCR (most drugs target TMRs)
natural target is NOT Hh ligand
agonists of Smo —> treat LOF Hh diseases
antagonists of Smo —> treat GOF Hh diseases
