Difference between revisions of "Macromolecular Crystallography"

Latest revision as of 10:44, 10 March 2017

Macromolecular Crystallography (sometimes abbreviated as MX) is the measurement of single-crystal diffraction patterns, in order to solve for the three-dimensional structure of macromolecules. The sample-of-interest is almost always a protein (protein crystallography, PX). Macromolecular crystallography is thus a powerful tool for resolving the three-dimensional structure of proteins, including studying their conformational changes when binding small molecules, or associating with other proteins.

Literature

Chayen NE, Boggon TJ, Cassetta A, Deacon A, Gleichmann T, Habash J, Harrop SJ, Helliwell JR, Nieh YP, Peterson MR, Raftery J, Snell EH, Hädener A, Niemann AC, Siddons DP, Stojanoff V, Thompson AW, Ursby T, Wulff M Trends and Challenges in Experimental Macromolecular Crystallography Quarterly Reviews of Biophysics 1996, 29 (03), 227-278. doi: 10.1017/S0033583500005837
John R. Helliwell and Edward P. Mitchell Synchrotron radiation macromolecular crystallography: science and spin-offs IUCrJ 2015, 2 (2). doi: 10.1107/S205225251402795X

@@ Line 1: / Line 1: @@
-'''Macromolecular Crystallography''' (sometimes abbreviated as '''MX''') is the measurement of single-crystal [[diffraction]] patterns, in order to solve for the three-dimensional structure of macromolecules. The sample-of-interest is almost always a protein. Macromolecular [[crystallography]] is thus a powerful tool for resolving the three-dimensional structure of proteins, including studying their conformational changes when binding small molecules, or associating with other proteins.
+'''Macromolecular Crystallography''' (sometimes abbreviated as '''MX''') is the measurement of single-crystal [[diffraction]] patterns, in order to solve for the three-dimensional structure of macromolecules. The sample-of-interest is almost always a protein ('''protein crystallography''', '''PX'''). Macromolecular [[crystallography]] is thus a powerful tool for resolving the three-dimensional structure of proteins, including studying their conformational changes when binding small molecules, or associating with other proteins.
 ==Literature==
 * Chayen NE, Boggon TJ, Cassetta A, Deacon A, Gleichmann T, Habash J, Harrop SJ, Helliwell JR, Nieh YP, Peterson MR, Raftery J, Snell EH, Hädener A, Niemann AC, Siddons DP, Stojanoff V, Thompson AW, Ursby T, Wulff M [http://journals.cambridge.org/action/displayAbstract?fromPage=online&aid=4858924&fileId=S0033583500005837 Trends and Challenges in Experimental Macromolecular Crystallography] ''Quarterly Reviews of Biophysics'' '''1996''', 29 (03), 227-278. [http://dx.doi.org/10.1017/S0033583500005837 doi: 10.1017/S0033583500005837]
 *  John R. Helliwell and Edward P. Mitchell [http://journals.iucr.org/m/issues/2015/02/00/fs5088/index.html Synchrotron radiation macromolecular crystallography: science and spin-offs] ''IUCrJ'' '''2015''', 2 (2). [http://dx.doi.org/10.1107/S205225251402795X doi: 10.1107/S205225251402795X]
-===[[Serial Femtosecond Crystallography|Serial Crystallography]] using X-ray Free-Electron Lasers ([[XFEL]]s)===
+===See Also===
-* Chapman et al. [http://www.nature.com/nature/journal/v470/n7332/full/nature09750.html Femtosecond X-ray protein nanocrystallography] ''Nature'' '''2011''', 470, 73-77. [http://dx.doi.org/10.1038/nature09750 doi: 10.1038/nature09750]
+* [[Serial Femtosecond Crystallography|Serial Crystallography]] using X-ray Free-Electron Lasers ([[XFEL]]s)
-*  Ilme Schlichting [http://journals.iucr.org/m/issues/2015/02/00/it5004/index.html Serial femtosecond crystallography: the first five years] ''IUCrJ'' '''2015''', 2 (2). [http://dx.doi.org/10.1107/S205225251402702X doi: 10.1107/S205225251402702X]
 ==See Also==

Difference between revisions of "Macromolecular Crystallography"

Latest revision as of 10:44, 10 March 2017

Literature

See Also

See Also

Navigation menu

Personal tools

Namespaces

Variants

Views

More

Search

Navigation

Tools