Amyotrophic lateral sclerosis (ALS) is a progressive neurodegenerative disease defined by motor neuron loss. Transgenic mouse model (Tg SOD1G93A) shows pathological features that closely mimic those seen in ALS patients. An hypothetic link between AD and ALS was suggested by finding an higher amount of amyloid precursor protein (APP) in the spinal cord anterior horn neurons, and of A beta peptides in ALS patients skin. In this work, we have investigated the expression of some genes involved in Alzheimer's disease, as APP, beta- and gamma-secretase, in an animal model of ALS, to understand some possible common molecular mechanisms between these two pathologies. For gene expression analysis, we carried out a quantitative RT-PCR in ALS mice and in transgenic mice over-expressing human wild-type SOD1 (Tg hSOD1). We found that APP and BACE1 mRNA levels were increased 1.5-fold in cortical cells of Tg SOD1G93A mice respect to Tg hSOD1, whereas the expression of gamma-secretase genes, as PSEN1, PSEN2, Nicastrin, and APH1a, showed no statistical differences between wild-type and ALS mice. Biochemical analysis carried out by immunostaining and western blotting, did not show any significant modulation of the protein expression compared to the genes, suggesting the existence of post-translational mechanisms that modify protein levels.

Spadoni, O., Crestini, A., Piscopo, P., Malvezzi Campeggi, L., Carunchio, I., Pieri, M., et al. (2009). Gene expression profiles of APP and BACE1 in Tg SOD1G93A cortical cells. CELLULAR AND MOLECULAR NEUROBIOLOGY, 29(5), 635-641 [10.1007/s10571-009-9356-8].

Gene expression profiles of APP and BACE1 in Tg SOD1G93A cortical cells

PIERI, MASSIMO;ZONA, CRISTINA;
2009-01-01

Abstract

Amyotrophic lateral sclerosis (ALS) is a progressive neurodegenerative disease defined by motor neuron loss. Transgenic mouse model (Tg SOD1G93A) shows pathological features that closely mimic those seen in ALS patients. An hypothetic link between AD and ALS was suggested by finding an higher amount of amyloid precursor protein (APP) in the spinal cord anterior horn neurons, and of A beta peptides in ALS patients skin. In this work, we have investigated the expression of some genes involved in Alzheimer's disease, as APP, beta- and gamma-secretase, in an animal model of ALS, to understand some possible common molecular mechanisms between these two pathologies. For gene expression analysis, we carried out a quantitative RT-PCR in ALS mice and in transgenic mice over-expressing human wild-type SOD1 (Tg hSOD1). We found that APP and BACE1 mRNA levels were increased 1.5-fold in cortical cells of Tg SOD1G93A mice respect to Tg hSOD1, whereas the expression of gamma-secretase genes, as PSEN1, PSEN2, Nicastrin, and APH1a, showed no statistical differences between wild-type and ALS mice. Biochemical analysis carried out by immunostaining and western blotting, did not show any significant modulation of the protein expression compared to the genes, suggesting the existence of post-translational mechanisms that modify protein levels.
2009
Pubblicato
Rilevanza internazionale
Articolo
Sì, ma tipo non specificato
Settore BIO/09 - FISIOLOGIA
English
Con Impact Factor ISI
Alzheimer; Amyotrophic lateral sclerosis; APP; BACE1; Tg SOD1G93A mice
Spadoni, O., Crestini, A., Piscopo, P., Malvezzi Campeggi, L., Carunchio, I., Pieri, M., et al. (2009). Gene expression profiles of APP and BACE1 in Tg SOD1G93A cortical cells. CELLULAR AND MOLECULAR NEUROBIOLOGY, 29(5), 635-641 [10.1007/s10571-009-9356-8].
Spadoni, O; Crestini, A; Piscopo, P; Malvezzi Campeggi, L; Carunchio, I; Pieri, M; Zona, C; Confaloni, A
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2108/45152
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