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Book ChapterDOI

Structure of serum albumin.

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TLDR
This chapter provides an insight of the findings of past significant papers with the current knowledge of the recently determined high resolution X-ray structure of serum albumin and suggests that AFP may have a higher affinity for some unknown ligands important for fetal development.
Abstract
Publisher Summary This chapter provides an insight of the findings of past significant papers with the current knowledge of the recently determined high resolution X-ray structure of serum albumin. The most outstanding property of albumin is its ability to bind reversibly an incredible variety of ligands. The sequences of all albumins are characterized by a unique arrangement of disulfide double loops that repeat as a series of triplets. Albumin belongs to a multigene family of proteins that includes α- fetoprotein (AFP) and vitamin D-binding protein (VDP), also known as G complement (Gc) protein. Although AFP is considered the fetal counterpart of albumin, its binding properties are distinct and it is suggested that AFP may have a higher affinity for some unknown ligands important for fetal development. Domain structure and the arrangement of the disulfides, the surface charge distribution, and the conformational flexibility of the albumin molecule are described. The nature of ligand binding, including small organics, long-chain fatty acids, and metals, to multiple sites on the albumin molecule is clearly depicted. The chapter concludes with the perceptive comments on future directions being taken to explore the structure and function of this fascinating protein.

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Citations
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Journal ArticleDOI

Albumin as a drug carrier: design of prodrugs, drug conjugates and nanoparticles.

TL;DR: This review gives an account of the different drug delivery systems which make use of albumin as a drug carrier with a focus on those systems that have reached an advanced stage of preclinical evaluation or that have entered clinical trials.
Journal ArticleDOI

Crystal structure of human serum albumin at 2.5 A resolution.

TL;DR: A new triclinic crystal form of human serum albumin (HSA), derived either from pool plasma or from a Pichia pastoris expression system, was obtained from polyethylene glycol 4000 solution, and three-dimensional structures of pHSA and rHSA were determined.
Journal ArticleDOI

Structure and reactivity of water at biomaterial surfaces

TL;DR: It is found that solvent properties of water within the interphase separating a solid surface from bulk water solution vary with contacting surface chemistry, and this interphase can extend tens of nanometers from a water-contacting surface due to a propagation of differences in self association between vicinal water and bulk-phase water.
Journal ArticleDOI

Crystal structure of human serum albumin complexed with fatty acid reveals an asymmetric distribution of binding sites

TL;DR: The crystal structure of HSA complexed with five molecules of myristate at 2.5 Å resolution is determined and it is shown that fatty acid molecules bind in long, hydrophobic pockets capped by polar side chains, many of which are basic.
Journal ArticleDOI

Human serum albumin: from bench to bedside.

TL;DR: HSA is a valuable biomarker of many diseases, including cancer, rheumatoid arthritis, ischemia, post-menopausal obesity, severe acute graft-versus-host disease, and diseases that need monitoring of the glycemic control.
References
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Journal ArticleDOI

Mn++ binding by plasma proteins.

TL;DR: Mn2+added to human or rabbit plasma in vitro combines selectively with the albumin fraction at pH 7.0 and Zn2+, Ni2+ and Co2+ can compete effectively for these sites.
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Interaction of albumin and fusidic acid: Appendix on interaction of albumin and fusidic acid

TL;DR: It is concluded that for albumin bound drugs the ‘storage depot’ of the organism also includes the fluid of the tissue spaces including the inflammatory oedema and an extravascular albumin pool similar in size to the plasma pool should not be neglected.
Journal ArticleDOI

Protein binding methodology: comparison of equilibrium dialysis and frontal analysis chromatography in the study of salicylate binding

TL;DR: The reproducibility of the data provided by GELFAC was far superior to that obtained with ED in spite of the fact that in both cases radioassay was employed, and analytical errors and bag binding did not appear to be contributory factors to the poor reproducability of the ED data.
Journal ArticleDOI

Alloalbuminemia in Sweden: structural study and phenotypic distribution of nine albumin variants

TL;DR: The high frequency and relatively uniform geographic distribution of the Arg-2----Cys mutation suggest that it may have occurred in a founder individual many generation ago in Sweden.