Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
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Query: UMLS:C0001486 (
Adenovirus
)
3,125
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Apolipoprotein E
(
apoE
)-deficient mice develop marked hyperlipidemia as well as atherosclerosis and thus are an excellent animal model for evaluating the potential for gene therapy in human genetic dyslipoproteinemias. Recombinant adenovirus containing either human
apoE
(rAdv.
apoE
) or the reporter gene luciferase (rAdv.luc) were generated and infused intravenously in
apoE
-deficient mice with preinfusion plasma total cholesterol of 644 +/- 149 mg/dl an cholesterol rich VLDL/IDL. After a single infusion of rAdv.
apoE
, plasma concentrations of human
apoE
ranging from 1.5 to 650 mg/dl were achieved.
Adenovirus
-mediated
apoE
replacement resulted in normalization of the lipid and lipoprotein profile with markedly decreased total cholesterol (103 +/- 18mg/dl), VLDL, IDL, and LDL, as well as increased HDL. Measurement of aortic atherosclerosis 1 mo after adenoviral infusion demonstrated a marked reduction in the mean lesion area of mice infused with rAdv.
apoE
(58 +/- 8 x 10(3) microns2) when compared with control mice infused with rAdv.luc (161 +/- 10 x 10(3) microns2; P < 0.0001). Thus,
apoE
expression for 4 wk was sufficient to markedly reduce atherosclerosis, demonstrating the feasibility of gene therapy for correction of genetic hyperlipidemias resulting in atherosclerosis. The combined use of adenovirus vectors and the
apoE
-deficient mouse represents a new in vivo approach that will permit rapid screening of candidate genes for the prevention of atherosclerosis.
...
PMID:Apolipoprotein E deficiency in mice: gene replacement and prevention of atherosclerosis using adenovirus vectors. 765 31
Apolipoprotein E
(
apoE
) promotes receptor-mediated catabolism of
apoE
-containing lipoprotein remnants. Impairments in remnant clearance are associated with type III hyperlipoproteinemia and premature atherosclerosis. In humans,
apoE
plasma levels correlate with plasma triglyceride levels, suggesting that excess
apoE
may also affect plasma triglyceride levels. We have used adenovirus-mediated gene transfer in mice to map the domains of
apoE
required for cholesterol and triglyceride clearance, in vivo.
Adenovirus
expressing apoE3 and apoE4 at doses of (1-2) x 10(9) pfu increased plasma cholesterol and triglyceride levels in normal C57BL6 mice and failed to normalize the high cholesterol levels of
apoE
-deficient mice due to induction of hypertriglyceridemia. In contrast, an adenovirus expressing the truncated
apoE
1-185 form normalized the cholesterol levels of E(-)(/)(-) mice and did not cause hypertriglyceridemia. Northern blot analysis of hepatic RNA from mice expressing the full-length and the truncated
apoE
forms showed comparable steady-state
apoE
mRNA levels of the full-length
apoE
forms that cause hyperlipidemia and the truncated
apoE
forms that do not cause hyperlipidemia. The findings suggest that the amino-terminal residues 1-185 of
apoE
are sufficient for the clearance of
apoE
-containing lipoprotein remnants by the liver, whereas domains of the carboxy-terminal one-third of
apoE
are required for
apoE
-induced hyperlipidemia.
...
PMID:The amino-terminal 1-185 domain of apoE promotes the clearance of lipoprotein remnants in vivo. The carboxy-terminal domain is required for induction of hyperlipidemia in normal and apoE-deficient mice. 1135 38
Recombinant
Adenovirus
and Adeno-associated virus (AAV) are highly effective vehicles for gene transfer into CNS cells. However, the duration of gene expression and the cytotoxicity to cells are quite different between these viral approaches. We initially investigated these distinctions by stereotaxically injecting both
Adenovirus
vector and AAV vectors expressing reporter genes into mouse hippocampus. The adenovirus vector induced a pronounced immune response with a marked increase in CD45 and MHC class I protein expression and transgene expression was shorter than six weeks. In contrast, with the AAV vector there was lower expression of CD45 and MHC class I immune activation markers, and longer expression of reporter gene (up to 12 months). To study the roles of human
Apolipoprotein E
(ApoE) alleles in the pathogenesis of Alzheimer's disease and other CNS diseases, we generated recombinant AAV-apoE alleles driven by the GFAP promoter and expressed them in the mouse brain of Alzheimer's disease mouse. High level ApoE expressions in mouse brain lasted for 12 months, and ApoE was specifically expressed in astrocytes. We demonstrate that AAV-GFAP-ApoE is valuable in studying the pathogenesis and in gene therapy for Alzheimer's disease and other CNS diseases.
...
PMID:Adeno-associated viral vector-mediated ApoE expression in Alzheimer's disease mice: low CNS immune response, long-term expression, and astrocyte specificity. 1497 65
