ABSTRACT
ABSTRACT BACKGROUND AND OBJECTIVES: Pro-inflammatory chemical mediators and algogenic substances seem to be confused by the sharing of their actions and by interactions in painful and inflammatory presentation. This study aimed at presenting a review of major inflammatory chemical mediators and place them in neuropathic pain pathophysiology. CONTENTS: Inflammation is the homeostatic response of vascularized tissues to remove harmful agents and restore their normal functions. Nervous system (central and/or peripheral) diseases and injuries may induce neuropathic pain and may also modify inflammatory process nervous mediation. In such pathological conditions, there might be pain without restrict link with admitedly harmful or painful stimuli, as well as there might be inflammation without restrict link with the presence of harmful agents and the need to remove them. Chemical mediators involved in neuropathic pain and inflammation pathophysiology modulate the presentation of both. CONCLUSION: Studies on inflammation offer evidences to support the important role of their chemical mediators in neuropathic pain pathogenesis. In peripheral and central sensitization, a thin borderline between reversibility or not of neuropathic pain may be respected or exceeded by inflammatory mediators actions.
RESUMO JUSTIFICATIVA E OBJETIVOS: Mediadores químicos pró-inflamatórios e substâncias algogênicas parecem se confundir pelo compartilhamento de suas ações e pelas interações no quadro doloroso e inflamatório. O objetivo deste estudo foi apresentar uma revisão sobre os principais mediadores químicos inflamatórios e situá-los na fisiopatologia da dor neuropática. CONTEÚDO: A inflamação é a resposta homeostática de tecidos vascularizados no sentido de remoção de agentes lesivos e restauro de suas funções normais. Doenças e lesões no sistema nervoso (central e/ou periférico) podem causar dor neuropática, e, também modificar a mediação nervosa do processo inflamatório. Nessas condições patológicas a dor pode ocorrer sem o vínculo restrito com estímulo reconhecidamente nocivo ou doloroso, assim como ocorrer quadro inflamatório sem o vínculo restrito com a presença de agentes lesivos e a necessidade de removê-los. Os mediadores químicos envolvidos na fisiopatologia da dor neuropática e da inflamação modulam o quadro de ambas. CONCLUSÃO: Os estudos sobre inflamação oferecem evidências para embasar a importância do papel dos seus mediadores químicos na patogênese da dor neuropática. Na sensibilização periférica e, também na central uma fronteira tênue entre a reversibilidade ou não do quadro neuropático pode ser respeitada ou ultrapassada pelas ações de mediadores inflamatórios.
ABSTRACT
PURPOSE: Coding variants in the optineurin gene (OPTN, GLC1E) have been reported to play a role in primary open-angle glaucoma (POAG) in various populations. This study investigated the role of OPTN sequence variants in patients with POAG in Ghana (West Africa). METHODS: This is a case-control study of unrelated Ghanaian POAG cases and non-glaucomatous controls. Ascertainment criteria for POAG included the presence of glaucomatous optic nerve neuropathy, associated visual field loss, and elevated intraocular pressure (IOP) in both eyes, all in the absence of secondary causes of glaucoma. Controls had normal optic nerves, visual fields, and IOP. All the coding exons of OPTN were polymerase chain reaction (PCR) amplified and sequenced in all 140 cases and 130 controls using an ABI 3730 DNA analyzer. RESULTS: All the coding exons of OPTN were sequenced in 140 POAG patients and 130 controls. Several coding variants were identified including M98K, A134A, V147L, P292P, A301G, S321S, and E322K. Three coding variants (V147L, P292P, and A301G) have not been reported previously. There were no significant differences on the frequencies of all the identified variants between POAG cases and controls in this population. CONCLUSIONS: This is the first comprehensive study of OPTN in a single West African population. Our results suggest that coding variants in OPTN may not contribute to the risk for POAG in persons of West African descent.
Subject(s)
Black People/genetics , Glaucoma, Open-Angle/genetics , Mutation/genetics , Open Reading Frames/genetics , Transcription Factor TFIIIA/genetics , Case-Control Studies , Cell Cycle Proteins , DNA Mutational Analysis , Gene Frequency , Ghana , Humans , Membrane Transport Proteins , Middle AgedABSTRACT
PURPOSE OF REVIEW: To review recent trends in genetic testing in medicine as they apply to newly evolving tests for patients with glaucoma. RECENT FINDINGS: The utilization of powerful molecular methods for genetic testing is now entering its early stages in the practice of medicine in general, and with testing, many issues, both medical and societal, have been raised. Only recently has testing for a disease risk factor in primary open angle glaucoma (POAG) become available. It is known that some mutations in the gene myocilin are associated with POAG. MYOC.mt1 is a relatively common promoter region variant in the myocilin gene for which there is a commercially available test. Some investigators have found that MYOC.mt1 may increase disease severity in patients with POAG, whereas others have not found this association. There is a need for further testing for the role of the MYOC.mt1 variant in the pathogenesis of POAG. SUMMARY: Genetic testing for glaucoma holds great promise. Currently available tests for disease-related tests in patients with glaucoma or at risk for this disease remain controversial.
