Synapsin I (SynI) and synapsin II (SynII) are major synaptic vesicle (SV) proteins that function in the regulation of the availability of SVs for release in mature neurons. SynI and SynII show a high level of sequence similarity and share many functions in vivo, although distinct physiological roles for the two proteins have been proposed. Both SynI-/- and SynII-/- mice have a normal lifespan, but exhibit a decreased number of SVs and synaptic depression upon high-frequency stimulation. Because of the role of the synapsin proteins in synaptic organization and plasticity, we studied the long-lasting effects of synapsin deletion on the phenotype of SynI-/- and SynII-/- mice during aging. Both SynI-/- and SynII-/- mice displayed behavioural defects that emerged during aging and involved emotional memory in both mutants, and spatial memory in SynII-/- mice. These abnormalities, which were more pronounced in SynII-/- mice, were associated with neuronal loss and gliosis in the cerebral cortex and hippocampus. The data indicate that SynI and SynII have specific and non-redundant functions, and that synaptic dysfunctions associated with synapsin mutations negatively modulate cognitive performances and neuronal survival during senescence.
Synapsin-I- and synapsin-II-null mice display an increased age-dependent cognitive impairment / Corradi, Anna; Zanardi, Alessio; Giacomini, Caterina; Onofri, Franco; Valtorta, Flavia; Zoli, Michele; Benfenati, Fabio. - In: JOURNAL OF CELL SCIENCE. - ISSN 0021-9533. - 121:18(2008), pp. 3042-3051. [10.1242/jcs.035063]
Synapsin-I- and synapsin-II-null mice display an increased age-dependent cognitive impairment
VALTORTA, FLAVIA;
2008-01-01
Abstract
Synapsin I (SynI) and synapsin II (SynII) are major synaptic vesicle (SV) proteins that function in the regulation of the availability of SVs for release in mature neurons. SynI and SynII show a high level of sequence similarity and share many functions in vivo, although distinct physiological roles for the two proteins have been proposed. Both SynI-/- and SynII-/- mice have a normal lifespan, but exhibit a decreased number of SVs and synaptic depression upon high-frequency stimulation. Because of the role of the synapsin proteins in synaptic organization and plasticity, we studied the long-lasting effects of synapsin deletion on the phenotype of SynI-/- and SynII-/- mice during aging. Both SynI-/- and SynII-/- mice displayed behavioural defects that emerged during aging and involved emotional memory in both mutants, and spatial memory in SynII-/- mice. These abnormalities, which were more pronounced in SynII-/- mice, were associated with neuronal loss and gliosis in the cerebral cortex and hippocampus. The data indicate that SynI and SynII have specific and non-redundant functions, and that synaptic dysfunctions associated with synapsin mutations negatively modulate cognitive performances and neuronal survival during senescence.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
