Effects of cyclosporin A administration on gene expression in rat brain

Abstract

Primary objective: The immunosuppressant cyclosporin A (CsA) is reported to have a strong anti-ischemic effect. Although this neuroprotective effect is speculated to be related to the blockade of a mitochondrial permeability transition pore (mPTP), the underlying molecular mechanism remains to be elucidated. This study focused on the effect of CsA on transcriptional regulation in brain cells.

Methods: CsA and a control substance were injected into rat brains and purified extracted mRNA. Both mRNAs were compared using a cDNA subtraction technique.

Results: Nine significantly up-regulated genes and seven significantly down-regulated genes were detected following CsA administration. All of the up-regulated genes are neurotrophic or reported to have roles in regeneration of brain tissue. Among the down-regulated genes, three are known to be detrimental to neuronal cells and are also reported to facilitate the pathology of Alzheimer's disease (AD) and four genes are related to oxidative metabolism.

Conclusions: Strong immunosuppression would present as a side-effect during CsA use as a neuroprotectant. The results of this study will help to discriminate between the CsA immunosuppressive effect and the neuroprotective effect at the molecular level and may lead to the development of new conceptual and pharmacological tools.

• Cyclosporin A
• brain ischemia
• neuroprotectant
• gene expression
• cDNA subtraction

Abbreviations
CsA	=	cyclosporin A
mPTP	=	mitochondrial permeability transition pore
AD	=	Alzheimer's disease
BAD	=	Bcl-associated death protein
CyPD	=	cyclophilin D
NFAT	=	Nuclear factor of activated T-cells
SSH	=	suppression subtractive hybridization
EF-1	=	Elongation factor-1
SCD2	=	Stearoyl-CoA desaturase 2
TCP1	=	T-complex protein 1
CCT	=	Chaperonin-containing TCP1
Fez1	=	fasciculation and elongation protein zeta 1
PKC	=	protein kinase C
TBP	=	TATA binding protein
TAF	=	TBP-associated factor
SPT	=	suppressor of yeast transposable elements
GCN	=	general control non-derepressible
GPR	=	G-protein-coupled receptor
dbEST	=	Database of Expressed Sequence Tags
CNS	=	central nervous system
HA	=	head activator
ZWINT	=	ZW10 interactor
rab	=	ras-related in brain
SNAP25	=	synaptosomal-associated protein 25
CCP	=	classical complement pathway
ER	=	endoplasmic reticulum
COP1	=	coat protein 1
MDH	=	Malate dehydrogenase
OXR1	=	oxidation resistance 1
AK3	=	Adenylate kinase 3
HIF1	=	hypoxia-inducible factor-1
PAS	=	Per/Arnt/Sim
PGK-1	=	Phosphoglycerate kinase 1
VILIP	=	Visinin-like Ca2 + binding protein.

Abbreviations
CsA	=	cyclosporin A
mPTP	=	mitochondrial permeability transition pore
AD	=	Alzheimer's disease
BAD	=	Bcl-associated death protein
CyPD	=	cyclophilin D
NFAT	=	Nuclear factor of activated T-cells
SSH	=	suppression subtractive hybridization
EF-1	=	Elongation factor-1
SCD2	=	Stearoyl-CoA desaturase 2
TCP1	=	T-complex protein 1
CCT	=	Chaperonin-containing TCP1
Fez1	=	fasciculation and elongation protein zeta 1
PKC	=	protein kinase C
TBP	=	TATA binding protein
TAF	=	TBP-associated factor
SPT	=	suppressor of yeast transposable elements
GCN	=	general control non-derepressible
GPR	=	G-protein-coupled receptor
dbEST	=	Database of Expressed Sequence Tags
CNS	=	central nervous system
HA	=	head activator
ZWINT	=	ZW10 interactor
rab	=	ras-related in brain
SNAP25	=	synaptosomal-associated protein 25
CCP	=	classical complement pathway
ER	=	endoplasmic reticulum
COP1	=	coat protein 1
MDH	=	Malate dehydrogenase
OXR1	=	oxidation resistance 1
AK3	=	Adenylate kinase 3
HIF1	=	hypoxia-inducible factor-1
PAS	=	Per/Arnt/Sim
PGK-1	=	Phosphoglycerate kinase 1
VILIP	=	Visinin-like Ca2 + binding protein.