Cryo-electron microscopy (cryo-EM) is a powerful microscopy-based technique used to study the structure and function of macromolecules. It allows scientists to look at proteins and other macromolecules at very high resolutions, far surpassing what can be achieved with other imaging techniques. Cryo-EM was first developed in the late 1970s and has since been revolutionizing structural biology, leading to breakthroughs in understanding the structure and function of proteins, viruses, and other macromolecules. Cryo-EM works by rapidly freezing samples in liquid ethane or liquid nitrogen at temperatures of -140°C to -180°C. This prevents the sample from being damaged by the electron beam and allows for more detailed imaging. The sample is then placed in an electron microscope, which sends a beam of electrons through it. The electrons interact with the sample and create a series of images that can be used to reconstruct a three-dimensional image of the sample. Cryo-EM is a powerful tool for structural biology and has been used to reveal the structure of many proteins and other macromolecules. It has also been used to study viruses and other pathogens. In addition, cryo-EM has been used to study protein-protein interactions, membrane proteins, and many other biological systems. Cryo-EM is becoming increasingly popular due to its ability to provide high-resolution images at a relatively low cost. It is also becoming easier to use, with automated data collection and software packages making it more accessible to a wider range of scientists.
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Maria Cecilia Colautti, Defense University of Republic of Argentina, Argentina
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