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  • Affinity chromatography  (2)
  • Civil and Mechanical Engineering  (1)
  • 1
    ISSN: 1612-1112
    Keywords: Affinity chromatography ; Biorecognition ; Proteins ; Polyacrylamide gels
    Source: Springer Online Journal Archives 1860-2000
    Topics: Chemistry and Pharmacology
    Notes: Summary Acrylamide and N,N′-methylenebisacrylamide were copolymerized in the presence of a protein to form a gel which was pressed through a sieve. The gel particles obtained were packed into a chromatographic tube. The experimental conditions for the polymerization are such that the pores of the gel particles are large enough to permit the protein to diffuse out of the particles, so that the entrapped protein can be removed from the bed by washing with an aqueous solution. However the interaction with the matrix is so strong that the protein can be desorbed only by a buffer containing 0.5 M sodium chloride or by a 10% solution of acetic acid containing 10% SDS. When a sample containing the protein present during the polymerization was applied to the column along with other proteins this protein was the only one adsorbed. The technique worked selectively with hemoglobin, cytochrome C and transferrin.
    Type of Medium: Electronic Resource
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  • 2
    ISSN: 1612-1112
    Keywords: Affinity chromatography ; Entrapment ; Molecular imprinting and recognition ; Proteins ; Selectivity and specificity
    Source: Springer Online Journal Archives 1860-2000
    Topics: Chemistry and Pharmacology
    Notes: Summary In a previous paper we presented preliminary experiments aimed at the preparation of gel particles with the property to recognize selectively some particular protein (hemoglobin, cytochrome C, transferrin) [1]. Using the same method we show in this article that human growth hormone, ribonuclease and myoglobin from horse can also be adsorbed specifically, indicating that the method may be universal or at least applicable to a great number of proteins. A gel with specific adsorption of three model proteins was synthesized in order to demonstrate that the beds can be employed to remove (traces of) several proteins contaminating a sample (“negative purification”). The degree of selective recognition is high, to judge from the fact that myoglobin from horse, but not that from whale, was adsorbed onto a column designed to bind specifically the former protein. This selectivity is noteworthy, since these two proteins have similar amino acid sequences and 3-D structures. The method for the synthesis of the specific gels involves polymerization of appropriate monomers (for instance acrylamide and its derivatives) in the presence of the protein to be adsorbed specifically, granulation of the gel formed, packing a column with the gel particles, washing the column to remove the protein and finally application of the sample for selective adsorption of the protein. The approach resembles that used for entrapment (immobilization) of proteins for affinity chromatography and that for molecular imprinting, with the distinct difference that the monomer composition is quite different and thereby the binding mechanism. This mechanism is discussed, for instance, in terms of (1) a new classification system for chromatographic beds based on the number of bonds between the solute and the matrix and the strength of each bond and (2) “non-specific bonds” (these bonds are often harmful in conventional chromatography, but we have used them to advantage). In this classification system the selective recognition is characterized by a large number of weak bonds. Therefore, so-called functional monomers are not used for the preparation of the gels because they often are charged and, accordingly, give rise to strong electrostatic interactions, i.e. the beds behave to some extent as ion-exchangers. In most experiments we have used a polyacrylamide gel with large pores to facilitate diffusion of proteins into and out of the gel granules. When used in chromatography these soft gels (which can be used repeatedly) allow only rather low flow rates. This problem can be overcome by a new approach to prepare the granules. Potential applications of the selective beds are discussed, as well as future improvements.
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  • 3
    Electronic Resource
    Electronic Resource
    New York, NY [u.a.] : Wiley-Blackwell
    International Journal for Numerical and Analytical Methods in Geomechanics 22 (1998), S. 425-447 
    ISSN: 0363-9061
    Keywords: closed-form solution ; transversely isotropic half-space ; Fourier transform ; Hankel transform ; rock anisotropy ; Engineering ; Civil and Mechanical Engineering
    Source: Wiley InterScience Backfile Collection 1832-2000
    Topics: Architecture, Civil Engineering, Surveying , Geosciences
    Notes: We rederive and present the complete closed-form solutions of the displacements and stresses subjected to a point load in a transversely isotropic elastic half-space. The half-space is bounded by a horizontal surface, and the plane of transverse isotropy of the medium is parallel to the horizontal surface. The solutions are obtained by superposing the solutions of two infinite spaces, one acting a point load in its interior and the other being free loading. The Fourier and Hankel transforms in a cylindrical co-ordinate system are employed for deriving the analytical solutions. These solutions are identical with the Mindlin and Boussinesq solutions if the half-space is homogeneous, linear elastic, and isotropic. Also, the Lekhnitskii solution for a transversely isotropic half-space subjected to a vertical point load on its horizontal surface is one of these solutions. Furthermore, an illustrative example is given to show the effect of degree of rock anisotropy on the vertical surface displacement and vertical stress that are induced by a single vertical concentrated force acting on the surface. The results indicate that the displacement and stress accounted for rock anisotropy are quite different for the displacement and stress calculated from isotropic solutions. © 1998 John Wiley & Sons, Ltd.
    Additional Material: 5 Ill.
    Type of Medium: Electronic Resource
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