| Literature DB >> 24877085 |
Simone Donati1, Simona Maria Caprani1, Giulia Airaghi1, Riccardo Vinciguerra1, Luigi Bartalena2, Francesco Testa3, Cesare Mariotti4, Giovanni Porta5, Francesca Simonelli3, Claudio Azzolini1.
Abstract
Vitreoretinal surgery has advanced in numerous directions during recent years. The removal of the vitreous body is one of the main characteristics of this surgical procedure. Several molecules have been tested in the past to fill the vitreous cavity and to mimic its functions. We here review the currently available vitreous substitutes, focusing on their molecular properties and functions, together with their adverse effects. Afterwards we describe the characteristics of the ideal vitreous substitute. The challenges facing every ophthalmology researcher are to reach a long-term intraocular permanence of vitreous substitute with total inertness of the molecule injected and the control of inflammatory reactions. We report new polymers with gelification characteristics and smart hydrogels representing the future of vitreoretinal surgery. Finally, we describe the current studies on vitreous regeneration and cell cultures to create new intraocular gels with optimal biocompatibility and rheological properties.Entities:
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Year: 2014 PMID: 24877085 PMCID: PMC4024399 DOI: 10.1155/2014/351804
Source DB: PubMed Journal: Biomed Res Int Impact factor: 3.411
Biochemical composition of the vitreous.
| Subgroups | Molecule | Action |
|---|---|---|
| Protein | Albumin (40%) | |
| Iron binding protein (30%) like transferrin | Protective effect to reduce iron toxicity | |
| Collagens | Structure of the vitreous | |
| Type II (60–70%) | ||
| Type IX (25%) | ||
| Type V/IX (10–25%) | ||
| Type IV (<10%) | ||
|
| ||
| Glycosaminoglycan | Hyaluronic acid (66–115 microgram/mL concentration) | Determine the vitreous body viscosity |
| Chondroitin sulfate | Major component of extracellular matrix | |
| Versican | ||
| Type IX collagen | ||
| Heparan sulfate | It maintains adequate spacing between the collagen fibrils | |
|
| ||
| Metabolites | Glucose | To support the enzymatic activity |
| Lactic acid | ||
| Ascorbic acid | Neovascularization inhibitor Increase proliferation of hyalocytes Potent antioxidant | |
| Amino acids | Metabolic cells maintenance | |
| Fatty acids unsaturated (50–55%) | Metabolic cells maintenance | |
| Prostaglandins (100 picogram/mL) | Cells regulation | |
| PGE2 | Cells regulation | |
| PGF2alpha | Cells regulation | |
| Prostacyclin | Cells regulation | |
| Thromboxane | Cells regulation | |
|
| ||
| Cells | Hyalocytes | Vitreous matrix creation and maintenance |
| Fibrocytes/fibroblasts | Vitreous matrix creation and maintenance | |
| Macrophages | Cells and matrix regulation and degradation | |
| Enzymes and metabolic activity: ACE | Cells regulation | |
Physical characteristics of the vitreous.
| Physical characteristics of the vitreous | |
|---|---|
| Weight | 4 g |
| Density | 1.0053–1.008 g/cm3 |
| Refractive index | 1.3345–1.3348 |
| Viscosity | 300–2000 cP |
| pH | 7.0–7.4 |
Characteristics of the ideal vitreous substitute.
| The ideal vitreous substitute | |
|---|---|
| Mimic the native vitreous | |
| Be easily manipulable during surgery | |
| Have similar viscoelastic proprieties | |
| Be clear and transparent | |
| Have refractive index and density similar to native vitreous | |
| Be biologically and chemically inert | |
| Be hydrophilic and insoluble in water | |
| Be able to maintain the IOP within a physiologic range and support the intraocular tissues in proper position | |
| Allow movement of ions and electrolytes and maintain the concentration of certain substances (oxygen, lactic acid, and ascorbic acid) | |
| Be clear | |
| Not induce toxic reactions | |
| Be biocompatible | |
| Be easily available, stable, and injectable through a small syringe | |
| Be able to maintain its light transparency post-op without undergoing opacification |