| Literature DB >> 27335891 |
Angela Patrizio1, Christian G Specht1.
Abstract
The ability to count molecules is essential to elucidating cellular mechanisms, as these often depend on the absolute numbers and concentrations of molecules within specific compartments. Such is the case at chemical synapses, where the transmission of information from presynaptic to postsynaptic terminals requires complex interactions between small sets of molecules. Be it the subunit stoichiometry specifying neurotransmitter receptor properties, the copy numbers of scaffold proteins setting the limit of receptor accumulation at synapses, or protein packing densities shaping the molecular organization and plasticity of the postsynaptic density, all of these depend on exact quantities of components. A variety of proteomic, electrophysiological, and quantitative imaging techniques have yielded insights into the molecular composition of synaptic complexes. In this review, we compare the different quantitative approaches and consider the potential of single molecule imaging techniques for the quantification of synaptic components. We also discuss specific neurobiological data to contextualize the obtained numbers and to explain how they aid our understanding of synaptic structure and function.Keywords: pair correlation analysis; photoactivated localization microscopy; single molecule localization microscopy; stochastic optical reconstruction microscopy
Year: 2016 PMID: 27335891 PMCID: PMC4891561 DOI: 10.1117/1.NPh.3.4.041805
Source DB: PubMed Journal: Neurophotonics ISSN: 2329-423X Impact factor: 3.593