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1. Introduction
2. Research interests
3. Learning objectives
4. Overview of the glutamatergic synapse
5. AMPARs and NMDARs
6. PSD-95 identification
7. PSD-95 structure
8. The role of PSD-95 in NMDAR clustering
9. Binding PSD-95 to endogenous NMDARs
10. Evidence for the role of PSD-95 in postsynaptic NMDAR localization (1)
11. Evidence for the role of PSD-95 in postsynaptic NMDAR localization (2)
12. Evidence for the role of PSD-95 in postsynaptic AMPAR localization (1)
13. Evidence for the role of PSD-95 in postsynaptic AMPAR localization (2)
14. PSD-95: a central organizer of the postsynaptic site
15. F-actin in dendritic spines
16. α-actinin co-immunoprecipitates with PSD-95
17. Kd124 reduces spine and synapse density
18. Kd124 reduces synapse density but not content of NMDARs of remaining synapses
19. Kd124 reduces content of PSD-95 in remaining synapses
20. Kd124 does not reduce content of GluA1
21. Kd124 does not reduce content of GluA2 or PSD-93
22. Kd124 reduces mEPSC frequency but not amplitude
23. Kd124 reduces synapse density but not content of glutamate receptors
24. α-actinin binding to the N-terminus of PSD-95
25. α-actinin binds to residues 1–13 of PSD-95
26. PSD-95 predicted interactions with CH2 and CH1
27. K10E and K11E mutations impair binding to α-actinin
28. K10E and K11E mutations reduce postsynaptic PSD-95 accumulation
29. K10E and K11E mutations reduce postsynaptic AMPAR accumulation (1)
30. K10E and K11E mutations reduce postsynaptic AMPAR accumulation (2)
31. E53K and E213K/D217K mutations
32. In summary of these results
33. Ca2+/CaM binding to PSD-95
34. Ca2+/CaM binds to 13 N-terminal residues
35. Ca2+/CaM binding and palmitoylation of PSD-95 (1)
36. Ca2+/CaM binding and palmitoylation of PSD-95 (2)
37. Y12E mutations affect Ca2+/CaM binding
38. K10E, K11E and Y12E mutations affect binding
39. Ca2+/CaM binding and palmitoylation of PSD-95 (3)
40. Ca2+/CaM displaced PSD-95 from spines
41. Ca2+/CaM displaced α-actinin from PSD-95
42. Threonine 19 (T19) phosphorylation
43. T19 phosphorylation augments and E17R decreases Ca2+/CaM binding
44. Palmitoylation of PSD-95 is reduced upon induction of chemical LTD
45. Abrogating Ca2+/CaM binding prevents depalmitoylation of PSD-95 during cLTD
46. Abrogating Ca2+/CaM binding to PSD-95 prevents loss of surface AMPARs during cLTD
47. Preventing depalmitoylation of PSD-95 during homeostatic synaptic downscaling
48. Preventing loss of surface AMPARs during homeostatic synaptic downscaling
49. Charge inversion mutations restore binding
50. Charge inversion mutations restore downscaling (1)
51. Charge inversion mutations restore downscaling (2)
52. Charge inversion mutations restore downscaling (3)
53. Ca2+/CaM regulates binding of PSD-95 to CDKL5
54. Ca2+/CaM regulates binding of PSD-95 to α-actinin
55. Ca2+ influx induces recruitment of Pyk2 by PSD-95
56. PSD-95 links the beta-adrenergic receptor to the AMPAR complex
57. Thank you for listening

Topics Covered

• PSD-95
• Structural proteins
• PSD-95 identification and structure
• Glutamatergic synapse
• PSD-95 anchors glutamate receptors
• Alpha-actinin anchors PSD-95
• AMPAR and NMDAR
• Alpha-actinin function and binding
• Ca2+/CaM binding to PSD-95
• Effect of Ca2+/CaM on PSD-95
• Palmitoylation/depalmitoylation cycle of PSD-95
• Long term depression (LTD)
• Homeostatic downscaling

Links

Series:

• Synapses, Neurotransmitters and Receptor Channels

Categories:

• Biochemistry
• Cell Biology
• Neuroscience

Therapeutic Areas:

• Neurology

Talk Citation

Publication History

• Published on July 31, 2022

Financial Disclosures

• Prof. Johannes Hell has not informed HSTalks of any commercial/financial relationship that it is appropriate to disclose.