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X-ray Crystallography &
its applications in Proteomics
Presented By : -
Akash Arora
X-ray crystallography is a technique used for determining the
atomic and molecular structure of a crystal, in which the
crystalline atoms cause a beam of incident X-rays to diffract into
many specific directions.
Then they use an X-ray beam to “hit” the crystallized molecule.
The electrons surrounding the molecule diffract as the X-rays hit
them. This forms a pattern, this type of pattern is called the X-ray
diffraction pattern.
Introduction
The English physicist Sir William Henry Bragg pioneered the
determination of crustal structure by X-ray diffraction
methods
X-ray crystallography is a complex field that has been
associated with several of science’s major breakthroughs in
the 20th century
Using X-ray crystal data, Dr. James Watson and Dr. Francis
Crick were able to determine the helix structure of DNA in
1953.
History
Why X-ray ??
Why crystal ??
Why X rays ?
 An electromagnetic wave of high energy and very short wavelength, which is able
to pass through many materials opaque to light.(wavelength 1 angstrom)
 The wavelength of X-ray photons is on the order of the distance between
atomic nuclei in solids (bonds are roughly 1.5-2.5 Å). You can think of it like
the waves fit nice between the atoms and "fill" the crystal.
Why Crystal ?
 Researchers crystallize an atom or molecule, because the precise position
of each atom in a molecule can only be determined if the molecule is
crystallized.
 If the molecule or atom is not in a crystallized form, the X-rays will
diffract unpredictably and the data retrieved will be too difficult if not
impossible to understand
X-ray diffraction
 Diffraction is the slight bending of light as it passes around the edge of an
object.
 X-ray crystallography uses the uniformity of light diffraction of crystals
to determine the structure of molecule or atom
 Then X-ray beam is used to hit the crystallized molecule.
 The electron surrounding the molecule diffract as the X-rays hit them.
 This forms a pattern. This type of pattern is known as X-ray diffraction
pattern.
Bragg’s Law
 There is a definite relationship between the angle at which a beam of X rays
must fall on the parallel planes of atoms in a crystal in order that there be
strong reflection, the wavelength of the X rays, and the distance between the
crystal planes
2d sinƟ = nλ
 Here d is the spacing between diffracting planes, Ɵ is the incident angle, n is
any integer, and λ is the wavelength of the beam.
 When an incident x-ray beam hits a scatterer, scattered x-rays are
emitted in all directions. Most of the scattering wave fronts are out of
phase interfere destructively. Some sets of wave fronts are in phase and
interfere constructively.
 A crystal is composed of many repeating unit cells in 3-dimensions, and
therefore, acts like a 3-dimensional diffraction grating. The
constructive interference from a diffracting crystal is observed as a
pattern of points on the detector. The relative positions of these points
are related mathematically to the crystal’s unit cell dimensions.
Destructive Interference Constructive Interference
Interference
 X-rays are scattered almost exclusively by the electrons in the atoms, not
by the nuclei.
 The incident electromagnetic wave exerts a force on the electrons. This
causes the electrons to oscillate with the same frequency as the incident
radiation. The oscillating electrons act as radiation scatters and emit
radiation at the same frequency as the incident radiation.
Interactions between X-rays and atoms
 The first-and often most difficult-step is to obtain
an adequate crystal of the material under study.
 The crystal should be sufficiently large (typically
larger than 0.1 mm in all dimensions), pure in
composition and regular in structure, with no
significant internal imperfections such as cracks.
 Researchers crystallize an atom or molecule,
because the precise position of each atom in a
molecule can only be determined if the molecule
is crystallized.
Procedure
 The crystal is placed in an intense beam of X-rays,
usually of a single wavelength (monochromatic X-
rays), producing the regular pattern of reflections.
As the crystal is gradually rotated, previous
reflections disappear and new ones appear; the
intensity of every spot is recorded at every
orientation of the crystal.
 Multiple data sets may have to be collected, with
each set covering slightly more than half a full
rotation of the crystal and typically containing tens
of thousands of reflections.
 In the third step, these data are combined
computationally with complementary chemical
information to produce and refine a model of the
arrangement of atoms within the crystal. The final,
refined model of the atomic arrangement-now called
a crystal structure is usually stored in a public
database.
 After the diffraction pattern is obtained, the data is
then processed by a computer and the structure of the
atom or molecule is deduced and visualized.
Instrumentation and
Limitations
Generally a typical x-ray diffraction contain below parts:
 X-ray source
 Detector
 Crystal on the end of mounting needle
 Liquid nitrogen steam to keep crystal cold
 Movable mount to rotate crystal
 Collimator
 X-ray Tube: the source of X Rays
 Incident-beam optics: condition the X-ray beam
before it hits the sample
 The goniometer: the platform that holds and
moves the sample, optics, detector, and/or tube
 The sample & sample holder
 Receiving-side optics: condition the X-ray beam
after it has encountered the sample
 Detector: count the number of X Rays scattered
by the sample.
Limitations
 Small-molecule crystallography typically involves crystals with fewer than
100 atoms in their asymmetric unit; such crystal structures are usually so
well resolved that the atoms can be discerned as isolated "blobs." of
electron density.
 By contrast, macromolecular crystallography often involves tens of
thousands of atoms in the unit cell. Such crystal structures are generally
less well-resolved (more "smeared out"); the atoms and chemical bonds
appear as tubes of electron density, rather than as isolated atoms.
 In general, small molecules are also easier to crystallize than
macromolecules; however, X-ray crystallography has proven possible even
for viruses with hundreds of thousands of atoms.
Application of X ray
Crystallography
 XRD is a nondestructive technique
 To identify crystalline phases and orientation
 To determine structural properties.
 To measure thickness of thin films and multi-layers
 To determine atomic arrangement
 X-ray diffraction is most widely used for the identification of unknown
crystalline materials (e.g. minerals, inorganic compounds). Determination of
unknown solids is critical to studies in geology, environmental science, material
science, engineering and biology.
 identification of fine-grained minerals such as clays and mixed layer clays that
are difficult to determine optically.
 determination of unit cell dimensions measurement of sample purity
Applications of X ray
Crystallography in proteomics
&
Conclusion
A branch of biotechnology concerned with applying the techniques of
molecular biology, biochemistry, and genetics to analyzing the structure,
function, and interactions of the proteins produced by the genes of a particular
cell, tissue, or organism, with organizing the information in databases, and with
applications of the data.
Proteomics
Protein Structure
Determination
Protein structure determination refers to finding the exact
orientations and arrangements of different amino acids
present in the protein.
X ray crystallography helps us to determine the structure of
proteins which further helps us to even determine its
function.
Protein Interaction
Studies
 Protein interaction refers to the way in which two or more proteins interact
with each other.
 Studies include the orientation, site of action and the major amino acids (of
protein) taking part in a particular reaction ray crystallography helps to
determine there Interactions.
Conformational
Studies
 It is necessary to determine the arrangements as it determines the structure
and function of Protein X ray crystallography is an efficient technique to
determine it.
 Conformational studies refers to spatial arrangements of atoms in a molecule
that can come about through free rotation of atoms about a chemical bond.
Enzyme catalysis
Determination
 Enzymes are protein. Determination of structure (specially active
site’s) and type of amino acids present in active sites determines
catalytic activities, Interaction level of enzymes.
 X ray crystallography helps us to determine and predict the
catalytic efficiency of enzymes.
 X-ray crystallography is essentially a form of very high resolution microscopy.
 It enables us to visualize protein structures at the atomic level and enhances our
understanding of protein function.
 Specifically we can study how proteins interact with other molecules, how they
undergo conformational changes, and how they perform catalysis in the case of
enzymes.
 Armed with this information we can design novel drugs that target a particular
protein, or rationally engineer an enzyme for a specific industrial process.
Conclusion
References
 https://www.jic.ac.uk/staff/david-lawson/xtallog/summary.htm
 https://en.wikipedia.org/wiki/X-ray_crystallography
 https://www.youtube.com/watch?v=gLsC4wlrR2A
 https://www.stolaf.edu/people/hansonr/mo/x-ray.html
 theconversation.com/explainer-what-is-x-ray-crystallography-22143
 Lehninger Principles of Biochemistry
Book by Albert L. Lehninger, David L. Nelson, and Michael M. Cox
 https://en.wikibooks.org/wiki/Structural_Biochemistry
X-ray Crystallography & Its Applications in Proteomics

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X-ray Crystallography & Its Applications in Proteomics

  • 1. X-ray Crystallography & its applications in Proteomics Presented By : - Akash Arora
  • 2. X-ray crystallography is a technique used for determining the atomic and molecular structure of a crystal, in which the crystalline atoms cause a beam of incident X-rays to diffract into many specific directions. Then they use an X-ray beam to “hit” the crystallized molecule. The electrons surrounding the molecule diffract as the X-rays hit them. This forms a pattern, this type of pattern is called the X-ray diffraction pattern. Introduction
  • 3. The English physicist Sir William Henry Bragg pioneered the determination of crustal structure by X-ray diffraction methods X-ray crystallography is a complex field that has been associated with several of science’s major breakthroughs in the 20th century Using X-ray crystal data, Dr. James Watson and Dr. Francis Crick were able to determine the helix structure of DNA in 1953. History
  • 4. Why X-ray ?? Why crystal ??
  • 5. Why X rays ?  An electromagnetic wave of high energy and very short wavelength, which is able to pass through many materials opaque to light.(wavelength 1 angstrom)  The wavelength of X-ray photons is on the order of the distance between atomic nuclei in solids (bonds are roughly 1.5-2.5 Å). You can think of it like the waves fit nice between the atoms and "fill" the crystal.
  • 6. Why Crystal ?  Researchers crystallize an atom or molecule, because the precise position of each atom in a molecule can only be determined if the molecule is crystallized.  If the molecule or atom is not in a crystallized form, the X-rays will diffract unpredictably and the data retrieved will be too difficult if not impossible to understand
  • 7.
  • 8. X-ray diffraction  Diffraction is the slight bending of light as it passes around the edge of an object.  X-ray crystallography uses the uniformity of light diffraction of crystals to determine the structure of molecule or atom  Then X-ray beam is used to hit the crystallized molecule.  The electron surrounding the molecule diffract as the X-rays hit them.  This forms a pattern. This type of pattern is known as X-ray diffraction pattern.
  • 9. Bragg’s Law  There is a definite relationship between the angle at which a beam of X rays must fall on the parallel planes of atoms in a crystal in order that there be strong reflection, the wavelength of the X rays, and the distance between the crystal planes 2d sinƟ = nλ  Here d is the spacing between diffracting planes, Ɵ is the incident angle, n is any integer, and λ is the wavelength of the beam.
  • 10.  When an incident x-ray beam hits a scatterer, scattered x-rays are emitted in all directions. Most of the scattering wave fronts are out of phase interfere destructively. Some sets of wave fronts are in phase and interfere constructively.  A crystal is composed of many repeating unit cells in 3-dimensions, and therefore, acts like a 3-dimensional diffraction grating. The constructive interference from a diffracting crystal is observed as a pattern of points on the detector. The relative positions of these points are related mathematically to the crystal’s unit cell dimensions. Destructive Interference Constructive Interference Interference
  • 11.  X-rays are scattered almost exclusively by the electrons in the atoms, not by the nuclei.  The incident electromagnetic wave exerts a force on the electrons. This causes the electrons to oscillate with the same frequency as the incident radiation. The oscillating electrons act as radiation scatters and emit radiation at the same frequency as the incident radiation. Interactions between X-rays and atoms
  • 12.  The first-and often most difficult-step is to obtain an adequate crystal of the material under study.  The crystal should be sufficiently large (typically larger than 0.1 mm in all dimensions), pure in composition and regular in structure, with no significant internal imperfections such as cracks.  Researchers crystallize an atom or molecule, because the precise position of each atom in a molecule can only be determined if the molecule is crystallized. Procedure
  • 13.  The crystal is placed in an intense beam of X-rays, usually of a single wavelength (monochromatic X- rays), producing the regular pattern of reflections. As the crystal is gradually rotated, previous reflections disappear and new ones appear; the intensity of every spot is recorded at every orientation of the crystal.  Multiple data sets may have to be collected, with each set covering slightly more than half a full rotation of the crystal and typically containing tens of thousands of reflections.
  • 14.  In the third step, these data are combined computationally with complementary chemical information to produce and refine a model of the arrangement of atoms within the crystal. The final, refined model of the atomic arrangement-now called a crystal structure is usually stored in a public database.  After the diffraction pattern is obtained, the data is then processed by a computer and the structure of the atom or molecule is deduced and visualized.
  • 15.
  • 17. Generally a typical x-ray diffraction contain below parts:  X-ray source  Detector  Crystal on the end of mounting needle  Liquid nitrogen steam to keep crystal cold  Movable mount to rotate crystal  Collimator
  • 18.  X-ray Tube: the source of X Rays  Incident-beam optics: condition the X-ray beam before it hits the sample  The goniometer: the platform that holds and moves the sample, optics, detector, and/or tube  The sample & sample holder  Receiving-side optics: condition the X-ray beam after it has encountered the sample  Detector: count the number of X Rays scattered by the sample.
  • 19.
  • 20. Limitations  Small-molecule crystallography typically involves crystals with fewer than 100 atoms in their asymmetric unit; such crystal structures are usually so well resolved that the atoms can be discerned as isolated "blobs." of electron density.  By contrast, macromolecular crystallography often involves tens of thousands of atoms in the unit cell. Such crystal structures are generally less well-resolved (more "smeared out"); the atoms and chemical bonds appear as tubes of electron density, rather than as isolated atoms.  In general, small molecules are also easier to crystallize than macromolecules; however, X-ray crystallography has proven possible even for viruses with hundreds of thousands of atoms.
  • 21. Application of X ray Crystallography  XRD is a nondestructive technique  To identify crystalline phases and orientation  To determine structural properties.  To measure thickness of thin films and multi-layers  To determine atomic arrangement
  • 22.  X-ray diffraction is most widely used for the identification of unknown crystalline materials (e.g. minerals, inorganic compounds). Determination of unknown solids is critical to studies in geology, environmental science, material science, engineering and biology.  identification of fine-grained minerals such as clays and mixed layer clays that are difficult to determine optically.  determination of unit cell dimensions measurement of sample purity
  • 23. Applications of X ray Crystallography in proteomics & Conclusion
  • 24. A branch of biotechnology concerned with applying the techniques of molecular biology, biochemistry, and genetics to analyzing the structure, function, and interactions of the proteins produced by the genes of a particular cell, tissue, or organism, with organizing the information in databases, and with applications of the data. Proteomics
  • 25.
  • 26. Protein Structure Determination Protein structure determination refers to finding the exact orientations and arrangements of different amino acids present in the protein. X ray crystallography helps us to determine the structure of proteins which further helps us to even determine its function.
  • 27. Protein Interaction Studies  Protein interaction refers to the way in which two or more proteins interact with each other.  Studies include the orientation, site of action and the major amino acids (of protein) taking part in a particular reaction ray crystallography helps to determine there Interactions.
  • 28. Conformational Studies  It is necessary to determine the arrangements as it determines the structure and function of Protein X ray crystallography is an efficient technique to determine it.  Conformational studies refers to spatial arrangements of atoms in a molecule that can come about through free rotation of atoms about a chemical bond.
  • 29. Enzyme catalysis Determination  Enzymes are protein. Determination of structure (specially active site’s) and type of amino acids present in active sites determines catalytic activities, Interaction level of enzymes.  X ray crystallography helps us to determine and predict the catalytic efficiency of enzymes.
  • 30.  X-ray crystallography is essentially a form of very high resolution microscopy.  It enables us to visualize protein structures at the atomic level and enhances our understanding of protein function.  Specifically we can study how proteins interact with other molecules, how they undergo conformational changes, and how they perform catalysis in the case of enzymes.  Armed with this information we can design novel drugs that target a particular protein, or rationally engineer an enzyme for a specific industrial process. Conclusion
  • 31. References  https://www.jic.ac.uk/staff/david-lawson/xtallog/summary.htm  https://en.wikipedia.org/wiki/X-ray_crystallography  https://www.youtube.com/watch?v=gLsC4wlrR2A  https://www.stolaf.edu/people/hansonr/mo/x-ray.html  theconversation.com/explainer-what-is-x-ray-crystallography-22143  Lehninger Principles of Biochemistry Book by Albert L. Lehninger, David L. Nelson, and Michael M. Cox  https://en.wikibooks.org/wiki/Structural_Biochemistry