aging and the circadian clock dennie kim mcb186 13 december 2006

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AGING AND THE CIRCADIAN CLOCK DENNIE KIM MCB186 13 DECEMBER 2006

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Page 1: AGING AND THE CIRCADIAN CLOCK DENNIE KIM MCB186 13 DECEMBER 2006

AGING AND THE CIRCADIAN CLOCK

DENNIE KIMMCB186

13 DECEMBER 2006

Page 2: AGING AND THE CIRCADIAN CLOCK DENNIE KIM MCB186 13 DECEMBER 2006

LEVELS OF CONTROL

CHOU ET AL., 2003. J. NEURO 23(33)

Page 3: AGING AND THE CIRCADIAN CLOCK DENNIE KIM MCB186 13 DECEMBER 2006

CR, SIRT1, and NEURONAL CELL SURVIVAL

B.L. Tang, 2006. Neurobiology of Aging 27 (503)

Page 4: AGING AND THE CIRCADIAN CLOCK DENNIE KIM MCB186 13 DECEMBER 2006

DETERIORATION OF BIOLOGICAL RHYTHMS

NEURODEGENERATION ?

Bentivoglio et al. 2006

Page 5: AGING AND THE CIRCADIAN CLOCK DENNIE KIM MCB186 13 DECEMBER 2006

DETERIORATION OF BIOLOGICAL RHYTHMS

Hofman et al., 2006

Page 6: AGING AND THE CIRCADIAN CLOCK DENNIE KIM MCB186 13 DECEMBER 2006

NOT JUST IN THE SCN?

M. HOFMAN, 2000.

Page 7: AGING AND THE CIRCADIAN CLOCK DENNIE KIM MCB186 13 DECEMBER 2006

CR-INDUCED LIFESPAN EXTENSION

- and -

NEURONAL RESCUE?

Page 8: AGING AND THE CIRCADIAN CLOCK DENNIE KIM MCB186 13 DECEMBER 2006

Hypothesis 1: CR mice are protected from degeneration

of rhythmicity.

• Calorie restrict miceCONTROL(S): NORMAL DIET MOUSE, RESVERATROL-TREATED MOUSE, SIRT1-K/O MOUSE

• Measure rhythms/neuronal activity• Test entrainment

Page 9: AGING AND THE CIRCADIAN CLOCK DENNIE KIM MCB186 13 DECEMBER 2006

Hypothesis 2: Deterioration of Circadian Clock is a Problem of

Neurodegeneration

• If neurons of the SCN (or DMH/VLPO) die during aging, the number of connections made should decrease.

• Use retrograde/anterograde tracers to label neuronal connections in young and old mice.

• Similarly, compare old mice to CR “old” mice.

Page 10: AGING AND THE CIRCADIAN CLOCK DENNIE KIM MCB186 13 DECEMBER 2006

Hypothesis 3: SIRT1 Activation in SCN Neurons

Can Prevent Circadian Dysfunction.

• Create an temporally/transiently SIRT1-inducible transgenic mouse.

• Measure rhythms/SCN-neuronal activity compared to wt mouse.

• Western blot/In situ hybridization/Immunohistochemistry to show increased levels of SIRT1 in transgenic mouse.