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      Analytical techniques in pharmaceutical analysis: A review

      , ,
      Arabian Journal of Chemistry
      Elsevier BV

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          Discovering high-affinity ligands for proteins: SAR by NMR.

          A nuclear magnetic resonance (NMR)-based method is described in which small organic molecules that bind to proximal subsites of a protein are identified, optimized, and linked together to produce high-affinity ligands. The approach is called "SAR by NMR" because structure-activity relationships (SAR) are obtained from NMR. With this technique, compounds with nanomolar affinities for the FK506 binding protein were rapidly discovered by tethering two ligands with micromolar affinities. The method reduces the amount of chemical synthesis and time required for the discovery of high-affinity ligands and appears particularly useful in target-directed drug research.
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            FDA's policy statement for the development of new stereoisomeric drugs.

            (1991)
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              Near-infrared spectroscopy applications in pharmaceutical analysis.

              Near-infrared (NIR) spectroscopy is a fast and non-destructive analytical technique that offers many advantages for a broad range of industrial applications. In this work, we reviewed recent developments in the pharmaceutical domain where it can be applied from raw material identification to final product release. The characteristics of NIR allow the technique to be implemented as a process analytical technology (PAT). Moreover, recent instrumental developments open the perspectives of numerous applications in the NIR imaging area. After "Introduction", according to their subject, the applications are discussed in the parts "Identification", "Water content", "Assay" and "Other applications".
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                Author and article information

                Journal
                Arabian Journal of Chemistry
                Arabian Journal of Chemistry
                Elsevier BV
                18785352
                February 2017
                February 2017
                : 10
                :
                : S1409-S1421
                Article
                10.1016/j.arabjc.2013.04.016
                0ed067bd-9de0-48de-9f89-5b6fbaa54d1b
                © 2017
                History

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