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Journal of Materials Chemistry B Accepted Manuscript This is an Accepted Manuscript, which has been through the Royal Society of Chemistry peer review process and has been accepted for publication. Accepted Manuscripts are published online shortly after acceptance, before technical editing, formatting and proof reading. Using this free service, authors can make their results available to the community, in citable form, before we publish the edited article. We will replace this Accepted Manuscript with the edited and formatted Advance Article as soon as it is available. You can find more information about Accepted Manuscripts in the Information for Authors. Please note that technical editing may introduce minor changes to the text and/or graphics, which may alter content. The journal’s standard Terms & Conditions and the Ethical guidelines still apply. In no event shall the Royal Society of Chemistry be held responsible for any errors or omissions in this Accepted Manuscript or any consequences arising from the use of any information it contains. www.rsc.org/materialsB Page 1 of 11Journal Name Journal of Materials Chemistry B Dynamic Article Links ► Cite this: DOI: 10.1039/c0xx00000x www.rsc.org/xxxxxx ARTICLE TYPE Hemostatic polymers: concept, state of the art and perspectives Fabio di Lena*a Received (in XXX, XXX) Xth XXXXXXXXX 20XX, Accepted Xth XXXXXXXXX 20XX DOI: 10.1039/b000000x 5 This article presents a critical overview of the most significant developments in the use of polymers as Manuscript hemostatic agents. The materials have been divided into two groups, that is, naturally occurring and synthetic. Remarkable examples include collagen, chitosan, bovine serum albumin/glutaraldehyde hydrogels, poly(cyano acrylate)s and poly(alkylene oxide)s. The different mechanisms for their modes of action as well as the structural features that are believed to induce hemostasis are discussed. Finally, an 10 overview of the future challenges is given. Introduction inorganic species, e.g., zeolites, have also been developed. 9 These are microporous aluminosilicates with a high surface area that are Accepted The ancient Greeks were the first to give blood a scientific able to entrap large volumes of water into their pores. As a result, consideration. They found out that blood circulates 50 the coagulation factors and the platelets concentrate at the B 15 uninterruptedly thoughtout the body, that it can be venous (which bleeding site accelerating the hemostasis. Materials of this type they termed “dark”) and arterial (which they termed “red”), and are commercially available with the name QuikClot ®. Although that it is produced in the bone marrow. 1 Moreover, they cheaper than fibrin sealants, zeolite powders are not without conducted studies on blood coagulation 2 and discovered that the drawbacks. For example, they may cause thermal injuries due to application of certain plant (e.g., turpentine) and mineral (e.g., 3 55 the strong exothermic reaction with blood, may remain as a 20 alum) compounds on wounds favoured blood stagnation. The foreign body in the wound, and they are toxic for the eyes and the process was termed αἷµα (=haíma=blood) στάσις lungs. Hemostats based on fibrin glues and inorganic materials, (=stàsis=halting), that is, hemostasis. We now know that the however, are out of the scope of this article and will not be hemostatic effect of such compounds is a consequence of the discussed further. contraction, i.e., the stypsis, of tissue and blood vessels that they 60 In the sections below, after a discussion of the basic principles 25 cause. Chemistry of hemostasis, the various polymer-based hemostatic agents are Many of the theories above were revised and refined by described. A thorough and critical overview of their modes of ancient Romans, in particular by Galen of Pergamon, arguably action as well as of the structural features that are believed to the greatest physician of the antiquity. Galen’s views have induce hemostasis is given. Yet, the major challenges in the field dominated the European medicine until the XVII century, when 65 are discussed and the reasons why modern polymer chemistry can 30 his claims started to be questioned. It was, however, not until be helpful in facing them explained. Literature up to the 1905, with the seminal work of Morawitz, 4 that the theory of beginning of 2013 is covered. hemostasis as we know it today (vide infra ) began to take shape. Probably inspired by these studies, in 1909, Bergel described the Fundamentals of hemostasis topical use of fibrin powder to promote wound healing.5 The next Materials 35 milestone in the history of hemostatic materials was placed in Due to space limitation and the presence of excellent reviews 6 7 10-13 1944 by Cronkite and Tidrick , who independently reported on 70 in the literature, this section will give only an overview of early forms of fibrin glues by mixing fibrinogen and thrombin. In hemostasis. Hemostasis is a complex physiological process that of a matter of seconds, thrombin catalyses the conversion of takes place through the synergistic action of three phenomena: (i) fibrinogen into fibrin units, which assemble in a three- vasoconstriction or stypsis; (ii) platelet plug formation; and (iii) 8 40 dimensional network that seals the wound. Increasingly more blood coagulation or clotting. The three processes come in effective formulations of fibrin glues have followed in the 75 succession as described below. When a blood vessel ruptures, the subsequent years, resulting in the present generation of body releases natural styptics like thromboxane and epinephrine commercial sealants such as Tisseel ®, Beriplast ®, and Biocol ®. that stimulate, respectively, a local and a general Such glues, however, are costly and, despite various screening vasoconstriction. Vasoconstriction is the narrowing of blood 45 protocols, may transmit viral or prion agents because they are vessels following the contraction of small muscles in their walls. Journal obtained from pooled blood products. Hemostats based on 80 This reduces the blood flow and thus the blood loss. At the same This journal is © The Royal Society of Chemistry [year] [journal] , [year], [vol] , 00–00 | 1 Journal Name Journal of Materials Chemistry B Dynamic Article Links ►Page 2 of 11 Cite this: DOI: 10.1039/c0xx00000x www.rsc.org/xxxxxx ARTICLE TYPE Table 1 Modes of action of polymer hemostats according to literature data. Artificial clot Tissue Acceleration of Vasoconstriction Water absorption formation/blood adhesion/barrier coagulation cascade gelation formation Basic poly(amino Manuscript ● acid)s Collagen/gelatin ● ● Chitin/chitosan ● ● ● Chitosan/polylysine ● ● ● ● gel Hydrophobically Accepted ● modified chitosan B Oxidized cellulose ● a BSA /glutaraldehyde ● ● gel Polyphosphates ● Poly(cyano ● acrylate)s Chemistry Poly(acrylic acid) ● ● b Poloxamers ● c d PEO -b-PDHA ● c PEO /chitosan gel ● ● ● e SAP /chitosan ● ● ● ● blends Materials f g PLA /PCL /chitosan ● ● ● of blends h RADA16-I peptide ● Acrylic cationic ● ● hydrogels i GRGDS -tagged ● l m Journal PLGA -b-PLL -b- This journal is © The Royal Society of Chemistry [year] [journal] , [year], [vol] , 00–00 | 2 Page 3 of 11 Journal of Materials Chemistry B c PEO nanoparticles a Bovine serum albumin. b Poly(ethylene oxide-b-propylene oxide-b-ethylene oxide). c Poly(ethylene oxide). d Poly(dihydroxyacetone). e Super absorbent polymer such as starch–poly(sodium acrylate-co -acrylamide). f Polylactic acid. g Poly-ε-caprolactone. h 16-residue synthetic peptide; see text for further information. i Gly-Arg-Gly-Asp-Ser sequence. l Poly(lactic-co -glycolic) acid. m Poly( L-lysine). time, as soon as the blood enters in contact with the collagen 5 present in the outer shell of the vessel membrane, the platelets Current polymer-based hemostatic agents stick to collagen and become activated (contact pathway). Naturally occurring polymers Activated platelets release chemical messengers such as adenosine diphosphate and thromboxane, which cause the Basic poly(amino acid)s . In 1954, Katchalski and co-workers aggregation of more platelets at the site of injury and enhance the reported that basic poly-α-amino acids such as polylysine (1), 10 vascular contraction, respectively. As a result, a platelet plug is 60 polyornithine (2) and polyarginine (3) accelerate the conversion formed that physically prevents the blood from escaping the of fibrinogen into fibrin whereas polyaspartic, polyglutamic, and vessel. While all this is going on, the blood clotting mechanism polycysteic acids retard this reaction. 14 In a follow-up study Manuscript enters into action. This involves a series of coagulation factors – focused on polylysine, they proposed two possible mechanisms mostly serine proteases – interacting with each other in a cascade for this.15 In one, polylysine, because of its cationic nature, forms 15 reaction that results in the conversion of fibrinogen into fibrin 65 a complex with fibrinogen which is then more readily attacked by strands, which reinforce the platelet plug. The coagulation factors the clotting agents. In the other, it acts as a link between exist in the blood in an inactive state and, following the damage fibrinogen and the clotting agents. Miller later demonstrated that of a blood vessel, are activated according to two pathways: the polylysine influences the coagulation cascade by activating the intrinsic pathway and the extrinsic pathway. The extrinsic coagulation factor X. As said above, this catalyzes the 20 pathway is a chemically

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