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Titlebook: Non-Biological Complex Drugs; The Science and the Daan J.A. Crommelin,Jon S. B. de Vlieger Book 2015 Springer International Publishing Swi

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ts and procedures for the optimum design of bandpass sigma-delta (SD) A/D interfaces for mixed-signal chips in standard CMOS technologies. The book differs from others in the very detailed and in-depth coverage of switched-current (SI) errors, which supports the design of high performance SI chips.
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Introduction: Defining the Position of Non-Biological Complex Drugs, the category of ‘biologicals’. NBCDs were earlier defined as: medicinal products, not being a biological medicine, where the active substance is not a homo-molecular structure, but consists of different (closely related and often nanoparticulate) structures that cannot be isolated and fully quantit
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Polymeric Micellessually spherical nanoparticle with a hydrophobic core acting as a reservoir for poorly soluble active pharmaceutical ingredients (APIs) and a hydrophilic shell which provides colloidal stability and limits protein adsorption and opsonisation, resulting in long-circulation times. Since the physicoche
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Drug Nanocrystalsmilling) methods, or by a combination of such processes. Suspensions of nanocrystals contain excipients adsorbing to the nanocrystal surface stabilizing the suspension against aggregation by steric hindrance and electrostatic repulsion. The complexity of this type of non-biological complex drugs (NB
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Low Molecular Weight Heparins, Biological Drugs close to Non-Biological Complex Drugss obtained from mammalian tissues and they are closely related to non-biological complex drugs because of their heterogeneity and their complex characterization. LMWHs are highly sulfated glycosaminoglycans obtained by partial chemical or enzymatic depolymerization of unfractionated heparin, which i
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