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2. Investigation of associations of ARMS2, CD14, and TLR4 gene polymorphisms with wet age-related macular degeneration in a Greek population

Author

Sarli A, Skalidakis I, Velissari A, Koutsandrea C, Stefaniotou M, Petersen MB, Kroupis C, Kitsos G, and Moschos MM

Subjects
AMD, ARMS2, CD14, TLR4, SNPs, PCR-RFLP, Ophthalmology, RE1-994
Abstract

Antonia Sarli,1 Iosif Skalidakis,2 Aliki Velissari,1 Chryssanthi Koutsandrea,2 Maria Stefaniotou,3 Michael B Petersen,4,5 Christos Kroupis,1,* George Kitsos,3,* Marilita M Moschos2,* 1Department of Clinical Biochemistry, Attikon University General Hospital, 21st Department of Ophthalmology, “G. Gennimatas” General Hospital, Medical School, National and Kapodistrian University of Athens, Athens, 3Department of Ophthalmology, Ioannina University General Hospital, University of Ioannina, Ioannina, Greece; 4Department of Clinical Genetics, Aalborg University Hospital, Aalborg, Denmark; 5Department of Clinical Medicine, Aalborg University Hospital, Aalborg, Denmark *These authors contributed equally to this work Background: Age-related macular degeneration (AMD) is a multifactorial degenerative ocular disease that leads to loss of central vision. Functional gene polymorphisms have already been associated with the disease (for example, ARMS2 A69S, rs10490924).Aim: The goal of our study was to verify the correlation of the aforementioned ARMS2 variation with the disease, to examine, for the first time, the role of the CD14 C260T variation (rs2569190), and to investigate the association of two TLR4 polymorphisms (Asp299Gly or rs4986790 and Thr399Ile or rs4986791) in a Greek population with the wet form of AMD.Patients and methods: Genomic DNAs were isolated from blood samples of 103 healthy controls and 120 Greek patients with wet AMD who were age- and sex-matched, and all of whom were clinically evaluated. For the genotyping of all selected polymorphisms, polymerase chain reaction–restriction fragment length polymorphism analysis was performed.Results and conclusions: This study confirmed the association between the ARMS2 variation and AMD, detecting the T risk allele in a significantly higher frequency in the patient group, compared with the control subjects (45% vs 29.13%, P

Published
2017

4. Assessment of hydroxychloroquine maculopathy after cessation of treatment: an optical coherence tomography and multifocal electroretinography study

Author

Moschos MM, Nitoda E, Chatziralli IP, Gatzioufas Z, Koutsandrea C, and Kitsos G

Subjects
Therapeutics. Pharmacology, RM1-950
Abstract

Marilita M Moschos,1 Eirini Nitoda,1 Irini P Chatziralli,1 Zisis Gatzioufas,2 Chryssanthi Koutsandrea,1 George Kitsos3 1First Department of Ophthalmology, Medical School, National and Kapodistrian University of Athens, Athens, Greece; 2Swiss Eye Research Foundation, Orasis Eye Clinic, Reinach, Switzerland; 3Department of Ophthalmology, Medical School, University of Ioannina, Ioannina, Greece Objective: This study was conducted to evaluate the macular status of patients treated with hydroxychloroquine before and after cessation of treatment.Methods: Forty-two patients with systemic lupus erythematosus underwent ocular examination based on visual acuity evaluation, optical coherence tomography retinal thickness measurements, and multifocal electroretinography (mfERG) records at first visit. The tests were repeated 6 months after treatment withdrawal and compared to the findings at their first visit.Results: Mean visual acuity (measured in log minimum angle of resolution) of both eyes was statistically increased after hydroxychloroquine discontinuation (difference in means: 0.06 [P

Published
2015

5. Systematic review of the association between Alzheimer’s disease and chronic glaucoma

Author

Tsilis AG, Tsilidis KK, Pelidou SH, and Kitsos G

Subjects
Ophthalmology, RE1-994
Abstract

Alexandros G Tsilis,1 Konstantinos K Tsilidis,2 Sygkliti-Henrietta Pelidou,3 George Kitsos1 1Department of Ophthalmology, 2Department of Hygiene and Epidemiology, 3Department of Neurology, University of Ioannina School of Medicine, Ioannina, Greece Abstract: A potential association between Alzheimer’s disease (AD) and chronic glaucoma has been suggested but results of epidemiological studies have been inconsistent. Therefore, we performed a systematic review and critical appraisal of this literature. We searched systematically in PubMed from December 1964 to September 2013 and identified 239 articles potentially relevant for abstract and full-text review. Statistical heterogeneity (variability) across studies was evaluated using the Cochran Q test and the I2 statistic, and the Newcastle-Ottawa score was used to assess study quality. Ten studies were finally selected. Compared to non-demented participants, patients with AD had a statistically significant decreased risk of glaucoma but the results were very heterogeneous, and thus summary estimates were not reported (I2, 89%; Pheterogeneity,

Published
2014

6. Correlation of the intronic LOXL1 polymorphism rs11638944 with pseudoexfoliation syndrome and glaucoma in a Greek population

Author

Papadopoulou, M.-K. Chatziralli, I. Tzika, K. Chiras, D. Kitsos, G. Kroupis, C.

Abstract

Background: The purpose of this study is the development and validation of a novel and robust genotyping method for a new lysyl oxidase-like 1 (LOXL1) intronic polymorphism (rs11638944, C > G) and the investigation of its potential association with pseudoexfoliation syndrome (PXS) and pseudoexfoliation glaucoma (PXG) in a Greek population. Material and methods: 242 DNA samples from 49 PXS, 64 PXG, 50 primary open-angle glaucoma (POAG) patients and 79 healthy age-matched controls were analyzed. Novel methodologies were developed and optimized, in order to genotype the intronic LOXL1 polymorphism: a) a real-time qPCR and melting curve analysis in the Light Cycler platform for rapid and cost-effective analysis and, b) a conventional PCR-RFLP method for analysis of a small number of samples. In selected samples, validity was checked with the reference DNA Sequencing method. Results: The real-time qPCR methodology was reliable, demonstrating good efficiency, reproducibility, accuracy in genotyping (100% concordance with the PCR-RFLP method and DNA Sequencing), with good allele discrimination (Tm = 53.26°C for C allele, Tm = 61.83°C for G allele, ΔTm = 8.57°C). The results were characterized by Hardy–Weinberg equilibrium in all groups. An increase from 18% in healthy controls to 61% in PXS patients was detected for the G/G homozygote thus, the C allele is protective for PXS with OR = 0.22 (95%CI: 0.11–0.42, p

Published
2021

7. Facilitators and barriers to more timely treatment of aneurysmal subarachnoid haemorrhage across two tertiary referral centres in Australia.

Author

Nguyen T.P., Stirling C., Kitsos G., Jose K., Nichols L., Chandra R., Rehman S., Smith K., Mosley I., Lai L., Asadi H., Dubey A., Froelich J., Thrift A., Gall S., Nguyen T.P., Stirling C., Kitsos G., Jose K., Nichols L., Chandra R., Rehman S., Smith K., Mosley I., Lai L., Asadi H., Dubey A., Froelich J., Thrift A., and Gall S.

Abstract

Backgrounds: Delays in treatment of aSAH appear common but the causes are not well understood. We explored facilitators and barriers to timely treatment of aSAH. Method(s): We used a mixed-methods multiple case-study approach including in-depth interviews with stakeholders involved in individual aSAH cases, focusing on events from onset to treatment. Quantitative data were extracted from medical records including date and times. Within-case analysis identified barriers and facilitators in 4 phases (pre-hospital, presentation, transfer, in-hospital), which were triangulated with the quantified time in each phase to determine significant influencing factors. Finally, we conducted thematic analysis across cases in early (<12h) and delayed (>12h) treatment group using a case-study matrix. Result(s): Twenty-seven cases (74.1% female) with 89 interviewees were included. Median (IQR) time to treatment was 15.1 (9.0, 24.1) hours. Only 37% of cases had treatment within 12 hours of onset. Rigorous mixed-methods data analysis and synthesis allowed identification of key themes influencing timely treatment of aSAH. Early recognition of aSAH at onset and diagnosis, availability of resources for immediate in-hospital treatment, and good coordination across patients' pathway were key facilitators for treatment within 12 hours from onset. Lack of recognition of aSAH at onset and unavailability of resources for definitive treatment were major barriers implicated in delayed treatment. Conclusion(s): We used a new approach to the analysis and synthesis of data from a clinically focused multiple case study. Using a robust mixed-methods approach, we identified the most significant and potentially modifiable factors affecting more timely treatment of aSAH within 12 hours.

Published
2021

8. Factors influencing more timely treatment of aneurysmal subarachnoid haemorrhage across two tertiary referral centres in Australia: A mixed methods study.

Author

Nguyen T., Stirling C., Kitsos G., Jose K., Nichols L., Chandra R., Rehman S., Smith K., Mosley I., Lai L., Asadi H., Dubey A., Froelich J., Thrift A., Gall S., Nguyen T., Stirling C., Kitsos G., Jose K., Nichols L., Chandra R., Rehman S., Smith K., Mosley I., Lai L., Asadi H., Dubey A., Froelich J., Thrift A., and Gall S.

Abstract

Background and Aims: Delays in treatment of aSAH appear common but the causes are not understood. We explored facilitators and barriers to timely treatment of aSAH. Method(s): We used a mixed-methods multiple case study approach including in-depth interviews with stakeholders involved in individual aSAH cases, focusing on events from onset to treatment. Quantitative data were extracted from medical records including date and times. Within-case analysis identified barriers and facilitators in 4 phases (pre-hospital, presentation, transfer, in-hospital), which were then triangulated with the quantified time in each phase to determine significant influencing factors. Finally, we conducted thematic analysis across cases in early (<12h) and delayed (>12h) treatment group using a case-study matrix. Result(s): Twenty-seven cases (74.1% female) with 89 interviewees were included. Median (IQR) time to treatment was 15.1 (9.0, 24.1) hours. Only 37% of cases had treatment within 12 hours of onset. Rigorous mixed-methods data analysis and synthesis allowed identification of key themes influencing timely treatment of aSAH. Early 'recognition of aSAH' at onset and diagnosis, 'availability of resources' for immediate in-hospital treatment, and good 'coordination' across patients' pathway were key facilitators for treatment within 12 hours from onset. Lack of 'recognition of aSAH' at onset and 'unavailability of resources' for definitive treatment were major barriers implicated in delayed treatment. Conclusion(s): We provided a guidance to a new approach to the analysis and synthesis of data from a clinically focused multiple case study. Using a robust mixed-methods approach, we identified the most significant and potentially modifiable factors affecting more timely treatment of aSAH within 12 hours.

Published
2021

9. A mixed-method study of factors affecting time to treatment of aneurysmal subarachnoid haemorrhage across two tertiary referral centres.

Author

Nguyen T., Stirling C., Kitsos G., Nichols L., Chandra R., Rehman S., Smith K., Mosley I., Lai L., Asadi H., Dubey A., Froelich J., Thrift A., Gall S., Nguyen T., Stirling C., Kitsos G., Nichols L., Chandra R., Rehman S., Smith K., Mosley I., Lai L., Asadi H., Dubey A., Froelich J., Thrift A., and Gall S.

Abstract

Background and Aims: Delays in treatment of aSAH appear common but the causes are not well understood. We explored facilitators and barriers to timely treatment of aSAH. Method(s): We used a mixed-methods multiple case study approach including in-depth interviews with stakeholders involved in individual aSAH cases, focusing on events from onset to treatment. Quantitative data were extracted from medical records including date and times. Within-case analysis identified barriers and facilitators in 4 phases (prehospital, presentation, transfer, in-hospital), which then being triangulated with the quantified time in each phase to determine significant influencing factors. Finally, we conducted thematic analysis across cases in early (<12h) and delayed (>12h) treatment group using a case-study matrix. Result(s): Twenty-seven cases (74.1% female) with 89 interviewees were included. Median (IQR) time to treatment was 15.1 (9.0, 24.1) hours. Only 37% of cases had treatment within 12 hours of onset. Qualitative and quantitative data triangulation identified key themes influencing timely treatment of aSAH. Early recognition of aSAH and good coordination during pre-hospital and diagnosis phases, and availability of resources for treatment during in-hospital period were main facilitators for treatment within 12 hours from onset (Figure 1a). Lack of recognition of aSAH at onset and lack of resources for immediate in-hospital treatment were major barriers for more delayed treatment (Figure 1b). Conclusion(s): Using a robust mixed-methods approach, we identified the most significant factors affecting more timely treatment within 12 hours from onset of aSAH. The factors are potentially modifiable at the patient/health professional and health system level and may improve timely treatment of aSAH.

Published
2021

13. Intravitreal ranibizumab versus vitrectomy for recurrent vitreous haemorrhage after pars plana vitrectomy for proliferative diabetic retinopathy: a prospective study

Author

Chatziralli, I. Dimitriou, E. Theodossiadis, G. Bourouki, E. Bagli, E. Kitsos, G. Theodossiadis, P.

Subjects
genetic structures, sense organs, eye diseases
Abstract

Purpose: To compare prospectively intravitreal ranibizumab treatment and pars plana vitrectomy (PPV) in patients with recurrent vitreous haemorrhage (VH) due to proliferative diabetic retinopathy (PDR), who were previously treated with PPV. Methods: Participants in this prospective study were 37 patients (37 eyes) with PDR, previously treated with PPV. All patients presented recurrent VH and were treated with either ranibizumab (n = 18) or PPV (n = 19). All participants were examined at week 2 post-treatment and every month thereafter for 1 year. Main outcomes were the need of PPV, the rate of recurrence of VH and the change in visual acuity by the end of the 12-month follow-up. Results: At month 12, there was statistically significant improvement in visual acuity in both groups compared to baseline, but the two groups did not differ regarding the change in visual acuity. In ranibizumab group, two patients presented recurrent VH during the follow-up and one patient needed PPV to clear the VH by month 12. In PPV group, two patients had mild recurrent VH, which cleared itself. No statistically significant difference was noticed regarding the rate of recurrent VH and the need of PPV between the two groups. Conclusion: Intravitreal ranibizumab seems to be a safe and effective treatment alternative in patients with recurrent VH secondary to PDR, who had been previously treated with PPV. © 2019, Springer Nature B.V.

Published
2020

14. Association of MMP2-1306C/T Polymorphism with Ischemic Retinal Vein Occlusion

Author

Christodoulou, A. Bagli, E. Gazouli, M. Moschos, M.M. Kitsos, G.

Abstract

Purpose: To investigate the possible association of the matrix metalloproteinase 2 (MMP2)-1306C/T polymorphism with the risk of ischemic retinal vein occlusion (iRVO). Methods: A total of 69 patients with RVO were enrolled in this study (43 with non-iRVO and 26 with iRVO). All subjects were screened for hypertension, diabetes mellitus, hyperlipidemia, history of stroke, anticoagulant medication, smoking status and glaucoma. The genotyping of MMP2-1306C/T polymorphism was performed using PCR-RFLP-based methods. Results: MMP2-1306C/T T allele carriers (CT+TT) were statistically significant associated with a higher risk of iRVO compared to CC genotype in the overall RVO group (odds ratio = 3.91, p = 0.015, 95% confidence interval:1.30–11.79). Analysis, following stratification by age revealed that T allele carriers had a statistically significant increased risk of iRVO compared to C allele carriers only in RVO patients

Published
2020

17. Genetic polymorphisms associated with the prevalence of retinal vein occlusion in a Greek population

Author

Christodoulou, A. Bagli, E. Gazouli, M. Moschos, M.M. Kitsos, G.

Subjects
eye diseases
Abstract

Purpose: To investigate possible associations of single-nucleotide polymorphisms (SNPs) from five genes with branch retinal vein occlusion (BRVO) and central retinal vein occlusion (CRVO). Methods: A total of 69 patients with retinal vein occlusion-RVO (24 with BRVO and 45 with CRVO), and 82 controls, were enrolled in this study. All subjects were screened for hypertension, diabetes mellitus, hyperlipidemia, glaucoma, anticoagulant medication, smoking status and history of stroke. The genotyping of AGTR1-A1166C, adiponectin + 276 G/T, MMP2-1306C/T, Gpla/lla-C807T/G873A and VKORC1-G1639A polymorphisms was performed using restriction fragment length polymorphism or allele-specific polymerase chain reaction. Results: The percentage of the AGTR1-A1166C C allele carriers and Gpla/lla-C807T/G873A T/A carriers was significantly higher in the CRVO patients than in the controls (P = 0.00001 and P = 0.0004, respectively). At the multiple logistic regression analysis, the AGTR1-A1166C C allele carrier status and the Gpla/lla-C807T/G873A T/A allele carrier status were found to be associated with an increased risk of CRVO. Moreover, adiponectin + 276 G/T T allele carriers had a significantly increased risk of RVO in subjects ≥ 75 years old. There was no significant difference between the BRVO patients and controls concerning the genotype or the allele frequency distributions of these SNPs. The genotype distributions or allelic frequencies of the other evaluated polymorphisms did not significantly differ between the patients with RVO and the control subjects. Conclusions: AGTR1 A1166C and Gpla/lla C807T/G873A polymorphisms are likely to be risk factors for CRVO. Adiponectin + 276 G/T SNP is likely to predispose to RVO in older subjects. © 2019, Springer Nature B.V.

Published
2019

18. TCF4 and COL8A2 Gene Polymorphism Screening in a Greek Population of Late-onset Fuchs Endothelial Corneal Dystrophy

Author

Moschos, M.M. Diamantopoulou, A. Gouliopoulos, N. Droutsas, K. Bagli, E. Chatzistefanou, K. Kitsos, G. Kroupis, C.

Abstract

Background/Aim: Fuchs’ endothelial corneal dystrophy (FECD) is a hereditary, progressive, bilateral, and irreversible disorder of the corneal endothelium. The purpose of this study was to develop a novel, accurate and high-throughput real-time polymerase chain reaction (PCR) method and melting-curve analysis in order to genotype the rs613872 polymorphism in the transcription factor 4 (TCF4) gene and to implement it on a well-ascertained sample of 22 Greek FECD patients and 58 healthy individuals, age- and sex-matched. Patients and Methods: DNA was extracted from blood samples, which were screened with the DNA sequencing method in order to detect the g.31753T>G/p.L450W (rs8035192) and g.31767C>A/p.Q455K (rs8035191) mutations in a COL8A2 genomic region. Results: TCF4 risk G allele frequency increased to 48% in FECD patients compared to 17% in healthy-subjects [OR=4.82 (95% CI=1.98-11.73)]. No p.L450W and p.Q455K COL8A2 gene mutations were detected. Conclusion: We confirmed that rs613872 in the TCF4 gene is strongly and statistically associated with late-onset FECD in a Greek population. © 2019 International Institute of Anticancer Research. All rights reserved.

Published
2019

19. The choice of drainage device in complicated glaucomas: Comparing Ahmed and Baerveldt implants

Author

Moschos, M.M. Nitoda, E. Gouliopoulos, N. Androudi, S. Damaskos, C. Laios, K. Bagkli, E. Garmpis, N. Kitsos, G.

Subjects
genetic structures, eye diseases
Abstract

Background/Aim: Glaucoma is a chronic and progressive optic neuropathy which leads to deterioration of visual function. It is estimated to be the second leading cause of severe vision loss and blindness worldwide. Failure of anti-glaucoma medication to sufficiently reduce intraocular pressure (IOP) and poor compliance with medication are indications for glaucoma surgery, for example using glaucoma drainage devices. Our aim was to compare the surgical outcomes following the implantation of Ahmed FP7 and Baerveldt 350 drainage devices. Patients and Methods: Five hundred and fifty-two patients with primary or secondary glaucoma were enrolled in the study. All patients had a history of failed trabeculectomy or other intraocular surgery, and IOP ≥18 mm Hg. The implantation of Ahmed (266 patients) or Baerveldt (286 patients) devices was randomly performed in the patients, who were subsequently examined for a period of 5 years. Follow-up visits were scheduled 1 day; 1 week; 1, 3 and 6 months; and 1, 1.5, 2, 3, 4 and 5 years postoperatively. Results: Significant reduction of IOP was achieved in both groups. Ahmed valve (28.3±9.3, 13.4±6.9, 14.2±6 and 12.7±4.5 mmHg at baseline, 1, 3, and 5 years postoperatively, respectively) resulted in significantly greater IOP reduction compared to Baerveldt implant (29.6±10.1, 15.4±5.5, 14.5±5.5 and 14.7±4.4 mmHg at baseline, 1, 3, and 5 years postoperatively, respectively). © 2019 International Institute of Anticancer Research. All rights reserved.

Published
2019

23. Karl Stellwag von Carion (1823-1904) and his studies on clinical and pathological anatomy of ocular cancer

Author

Laios, K. Lagiou, E. Piagkou, M. Kitsos, G. Moschos, M.M.

Abstract

Karl Stellwag von Carion (1823-1904) was a very important figure of European ophthalmology during the 19th century. Besides his other contributions in ophthalmology such as ‘Stellwag sign', coining the term ‘ectopia lentis' for lens dislocation and fundamental studies on glaucoma, refraction, accommodation and light polarization, his studies on ocular cancer were very significant but not highlighted by modern research. © 2018 Firenze University Press.

Published
2018

24. Investigation of associations of ARMS2, CD14, and TLR4 gene polymorphisms with wet age-related macular degeneration in a Greek population

Author

Sarli, A. Skalidakis, I. Velissari, A. Koutsandrea, C. Stefaniotou, M. Petersen, M.B. Kroupis, C. Kitsos, G. Moschos, M.M.

Subjects
eye diseases
Abstract

Background: Age-related macular degeneration (AMD) is a multifactorial degenerative ocular disease that leads to loss of central vision. Functional gene polymorphisms have already been associated with the disease (for example, ARMS2 A69S, rs10490924). Aim: The goal of our study was to verify the correlation of the aforementioned ARMS2 variation with the disease, to examine, for the first time, the role of the CD14 C260T variation (rs2569190), and to investigate the association of two TLR4 polymorphisms (Asp299Gly or rs4986790 and Thr399Ile or rs4986791) in a Greek population with the wet form of AMD. Patients and methods: Genomic DNAs were isolated from blood samples of 103 healthy controls and 120 Greek patients with wet AMD who were age- and sex-matched, and all of whom were clinically evaluated. For the genotyping of all selected polymorphisms, polymerase chain reaction–restriction fragment length polymorphism analysis was performed. Results and conclusions: This study confirmed the association between the ARMS2 variation and AMD, detecting the T risk allele in a significantly higher frequency in the patient group, compared with the control subjects (45% vs 29.13%, P

Published
2017

25. Immunohistochemical study of vasculogenic mimicry and angiogenesis in melanocytic tumors of the eye and the periocular area

Author

Spiliopoulos, K. Peschos, D. Batistatou, A. Ntountas, I. Papoudou-Bai, A. Zioga, A. Agnantis, N. Kitsos, G.

Subjects
neoplasms
Abstract

Background/Aim: The ability of a tumor to grow requires a sufficient blood supply. Microvascular density is considered the standard for assessing the neovasculature. Tumor cell vasculogenic mimicry refers to the formation of tumor cell-lined vessels that contribute to tumor neovascularization. The aim of the present work was to study angiogenesis and vasculogenic mimicry in benign and malignant melanocytic tumors of the eye and the periocular region. Patients and Methods: Histological sections from 118 patients were studied. Eighty-eight of the patients had nevi while the remaining 30 had malignant melanomas. Microvascular density was assessed by using antibodies against the endothelial cell markers CD31 and CD34. Vascular-like channels between neoplastic cells, that were not lined by endothelial cells and thus were negative for CD31 and CD34, represented areas of vasculogenic mimicry. Results: Angiogenesis was more pronounced in melanomas compared to melanocytic nevi and was increased in melanomas with high mitotic index and/or epithelioid cell preponderance compared to melanomas with low mitotic index and/or spindle cell predominance. Vasculogenic mimicry was observed in many melanomas, while it was evident in the minority of benign nevi as well. Conclusion: The existence of vasculogenic mimicry in benign nevi might have prognostic implications.

Published
2017

26. Assessment of hydroxychloroquine maculopathy after cessation of treatment: An optical coherence tomography and multifocal electroretinography study

Author

Moschos, M.M. Nitoda, E. Chatziralli, I.P. Gatzioufas, Z. Koutsandrea, C. Kitsos, G.

Subjects
genetic structures, sense organs, eye diseases
Abstract

Objective: This study was conducted to evaluate the macular status of patients treated with hydroxychloroquine before and after cessation of treatment. Methods: Forty-two patients with systemic lupus erythematosus underwent ocular examination based on visual acuity evaluation, optical coherence tomography retinal thickness measurements, and multifocal electroretinography (mfERG) records at first visit. The tests were repeated 6 months after treatment withdrawal and compared to the findings at their first visit. Results: Mean visual acuity (measured in log minimum angle of resolution) of both eyes was statistically increased after hydroxychloroquine discontinuation (difference in means: 0.06 [P

Published
2015

28. Proximal 10q duplication in a child with severe central hypotonia characterized by array- comparative genomic hybridization: A case report and review of the literature

Author

Manolakos, E. Vetro, A. Garas, A. Thomaidis, L. Kefalas, K. Kitsos, G. Ziegler, M. Liehr, T. Zuffardi, O. Papoulidis, I.

Abstract

Proximal 10q duplication is a well- defined but rare genetic syndrome. Duplication of proximal segments of the long arm of chromosome 10 results in a pattern of malformations, which are distinct from those of the more common distal 10q trisomy syndrome. The present study describes the case of a boy with phenotypic abnormalities (severe central hypotonia, mild ataxia, moderate developmental delay and mild dysmorphic features), due to duplication of chromosome region, 10q11.21→q11.22, which was characterized by the array- comparative genomic hybridization (CGH) technique. The phenotypic findings were compared with those in eight additional similar published cases. Major similarities have emerged, suggesting a likely minimal critical region. However, only detailed characterization of additional cases may provide firm conclusions.

Published
2014

29. A de novo 2.9 Mb interstitial deletion at 13q12.11 in a child with developmental delay accompanied by mild dysmorphic characteristics

Author

Lagou, M. Papoulidis, I. Orru, S. Papadopoulos, V. Daskalakis, G. Kontodiou, M. Anastasakis, E. Petersen, M.B. Kitsos, G. Thomaidis, L. Manolakos, E.

Subjects
congenital, hereditary, and neonatal diseases and abnormalities
Abstract

Background: Proximal deletions in the 13q12.11 region are very rare. Much larger deletions including this region have been described and are associated with complex phenotypes of mental retardation, developmental delay and various others anomalies. Results: We report on a 3-year-old girl with a rare 2.9 Mb interstitial deletion at 13q12.11 due to a de novo unbalanced t(13;14) translocation. She had mild mental retardation and relatively mild dysmorphic features such as microcephaly, flat nasal bridge, moderate micrognathia and clinodactyly of 5th finger. Molecular karyotyping revealed a deletion on the long arm of chromosome 13 as involving sub-bands 13q12.11, a deletion of about 2.9 Mb. Discussion: The clinical application of array-CGH has made it possible to detect submicroscopical genomic rearrangements that are associated with varying phenotypes.The description of more patients with deletions of the 13q12.11 region will allow a more precise genotype-phenotype correlation. © 2014 Lagou et al.

Published
2014

32. Development of novel LOXL1 genotyping method and evaluation of LOXL1, APOE and MTHFR polymorphisms in exfoliation syndrome/glaucoma in a Greek population

Author

Chiras, D., Tzika, K., Kokotas, H., Oliveira, S. C., Grigoriadou, M., Kastania, A., Dima, K., Stefaniotou, M., Aspiotis, M., Petersen, M. B., Christos Kroupis, and Kitsos, G.

Subjects
Male, Genotyping Techniques, Greece, Molecular Sequence Data, Reproducibility of Results, Exfoliation Syndrome, Nucleic Acid Denaturation, Polymorphism, Single Nucleotide, Apolipoproteins E, Case-Control Studies, Humans, Female, Amino Acid Oxidoreductases, Amino Acid Sequence, Glaucoma, Open-Angle, Methylenetetrahydrofolate Reductase (NADPH2), Aged
Abstract

In the Greek population of Epirus, exfoliation syndrome (XFS) and exfoliation glaucoma (XFG) occur at a high prevalence. In this study, we validate a novel lysyl oxidase-like 1 (LOXL1) genotyping method, investigate the previously reported association of LOXL1 with XFS/XFG, and evaluate apolipoprotein E (APOE) and methylenetetrahydrofolate reductase (MTHFR) polymorphisms as genetic risk factors for both conditions in our population.

Published
2013

33. Biomarkers in primary open angle glaucoma

Author

Kokotas, H. Kroupis, C. Chiras, D. Grigoriadou, M. Lamnissou, K. Petersen, M.B. Kitsos, G.

Subjects
genetic structures, sense organs, eye diseases
Abstract

Glaucoma, a leading cause of blindness worldwide, is currently defined as a disturbance of the structural or functional integrity of the optic nerve that causes characteristic atrophic changes in the optic nerve, which may lead to specific visual field defects over time. This disturbance usually can be arrested or diminished by adequate lowering of intraocular pressure (IOP). Glaucoma can be divided roughly into two main categories, ' open angle ' and ' closed angle ' glaucoma. Open angle, chronic glaucoma tends to progress at a slower rate and patients may not notice loss of vision until the disease has progressed significantly. Primary open angle glaucoma (POAG) is described distinctly as a multifactorial optic neuropathy that is chronic and progressive with a characteristic acquired loss of optic nerve fibers. Such loss develops in the presence of open anterior chamber angles, characteristic visual field abnormalities, and IOP that is too high for the healthy eye. It manifests by cupping and atrophy of the optic disc, in the absence of other known causes of glaucomatous disease. Several biological markers have been implicated with the disease. The purpose of this study was to summarize the current knowledge regarding the non-genetic molecular markers which have been predicted to have an association with POAG but have not yet been validated. Copyright © 2012 by Walter de Gruyter.

Published
2012

36. Primary open angle glaucoma due to T377M MYOC: Population mapping of a Greek founder mutation in Northwestern Greece

Author

Kitsos, G. Petrou, Z. Grigoriadou, M. Samples, J.R. Hewitt, A.W. Kokotas, H. Giannoulia-Karantana, A. Mackey, D.A. Wirtz, M.K. Moschou, M. Ioannidis, J.P.A. Petersen, M.B.

Subjects
genetic structures, eye diseases
Abstract

Background: Mutations in the MYOC gene have been shown to explain 5% of unrelated primary open angle glaucoma (POAG) in different populations. In particular, the T377M MYOC mutation has arisen at least three separate times in history, in Great Britain, India, and Greece. The purpose of this study is to investigate the distribution of the mutation among different population groups in the northwestern region of Greece. Materials and methods: We explored the distribution of the "Greek" T377M founder mutation in the Epirus region in Northwestern Greece, which could be its origin. Genotyping was performed in POAG cases and controls by PCR amplification of the MYOC gene, followed by digestion with restriction enzyme. Statistical analyses were performed by an exact test, the Kaplan-Meier method and the t-test. Results: In the isolated Chrysovitsa village in the Pindus Mountains, a large POAG family demonstrated the T377M mutation in 20 of 66 family members while no controls from the Epirus region (n = 124) carried this mutation (P < 0.001). Among other POAG cases from Epirus, 2 out of 14 familial cases and 1 out of 80 sporadic cases showed the mutation (P = 0.057). The probability of POAG diagnosis with advancing age among mutation carriers was 23% at age 40, and reached 100% at age 75. POAG patients with the T377M mutation were diagnosed at a mean age of 51 years (SD ± 13.9), which is younger than the sporadic or familial POAG cases: 63.1 (SD ± 11) and 66.8 (SD ± 9.8) years, respectively. Conclusions: The T377M mutation was found in high proportion in members of the Chrysovitsa family (30.3%), in lower proportion in familial POAG cases (14.2%) and seems rare in sporadic POAG cases (1.2%), while no controls (0%) from the Epirus region carried the mutation. Historical and geographical data may explain the distribution of this mutation within Greece and worldwide. © 2010 Kitsos et al, publisher and licensee Dove Medical Press Ltd.

Published
2010

37. Periocular xanthogranuloma: A forgotten entity?

Author

Papagoras, C., Kitsos, G., Voulgari, P. V., Zikou, A. K., Argyropoulou, M. I., Zioga, A., and Drosos, A. A.

Abstract

Periocular xanthogranulomatous diseases are a rare group of disorders which are characterized by a predilection to affect the orbit and ocular adnexa and special histopathological features, in particular infiltrates comprising non-Langerhans-derived foamy histiocytes and Touton giant cells. The differential diagnosis is difficult and occasionally definite diagnosis cannot be established even after clinical and histopathological findings are taken together. We describe a case of a middle-aged man who presented with a 10-year history of voluminous eyelid swelling with concomitant late-onset atopic manifestations, namely bronchial asthma and allergic rhinitis with nasal polyps. After thorough clinical and laboratory investigation, including a biopsy of the eyelid, we classified the patient's disease to a rare entity that has been relatively recently described: periocular xanthogranuloma associated with adult-onset asthma. In a review of the literature, no prospective trials concerning the treatment of this disease were found. The literature mainly contained case reports and case series in which corticosteroids and chemotherapy with alkylating agents have been reported to be beneficial. We treated our patient with a combination of oral corticosteroids and cyclophosphamide pulses and we observed substantial regression of the eyelid masses together with a normalization of systemic immunologic abnormalities. Clin Ophthalmol

Published
2010

38. Characterization of 23 small supernumerary marker chromosomes detected at pre-natal diagnosis: The value of fluorescence in situ hybridization

Author

Manolakos, E. Kefalas, K. Neroutsou, R. Lagou, M. Kosyakova, N. Ewers, E. Ziegler, M. Weise, A. Tsoplou, P. Rapti, S.-M. Papoulidis, I. Anastasakis, E. Garas, A. Sotiriou, S. Eleftheriades, M. Peitsidis, P. Malathrakis, D. Thomaidis, L. Kitsos, G. Orru, S. Liehr, T. Petersen, M.B. Kitsiou-Tzeli, S.

Abstract

Small supernumerary marker chromosomes (sSMCs) cannot be identified or characterized unambiguously by conventional cytogenetic banding techniques. Until recently, the large variety of marker chromosomes, as well as the limitations in their identification, have presented a diagnostic problem. In order to determine the origin of sSMCs, we used a variety of fluorescence in situ hybridization (FISH) methods, including centromere-specific multicolor FISH, acrocentric specific multicolor FISH, subcentromere-specific multicolor FISH and multicolor FISH with whole chromosome paint probes. Moreover, uniparental disomy testing was in all cases attempted. From a total of 28,000 pre-natal samples from four diagnostic genetics laboratories in Greece, 23 (0.082%) supernumerary marker chromosomes were detected. The mean maternal age was 36.2 years (range 27-43) and the mean gestational age at which amniocentesis was performed was 18.5 weeks (range 16-23). Eighteen markers were de novo and 5 markers were inherited. Molecular cytogenetic methods were applied to determine the chromosomal origin and composition of the sSMC. In total, 17 markers were derived from acrocentric chromosomes (14, 15, 21 and 22) and 6 markers were non-acrocentric, derived from chromosomes 9, 16, 18, 20 and Y. Uniparental disomy was not detected in any of the cases studied. With regard to pregnancy outcome, 13 pregnancies resulted in normal healthy neonates, while 10 pregnancies were terminated due to ultrasound abnormalities. A total of 23 marker chromosomes from 28,000 pre-natal samples (0.082%) were identified. Molecular cytogenetic techniques provided valuable information on the chromosomal origin and composition of all the sSMCs. Especially in cases with normal ultrasound, the FISH results rendered genetic counseling possible in a category of cases previously considered a diagnostic problem. Abnormal outcome was observed in 10 cases (43,5%), 7 of which showed abnormal ultrasound findings. New technologies, such as array-comparative genomic hybridiza-tion, should be used in future genotype-phenotype correlation studies, although the high mosaicism rate poses a problem.

Published
2010

39. The use of array-CGH in a cohort of Greek children with developmental delay

Author

Manolakos, E. Vetro, A. Kefalas, K. Rapti, S.-M. Louizou, E. Garas, A. Kitsos, G. Vasileiadis, L. Tsoplou, P. Eleftheriades, M. Peitsidis, P. Orru, S. Liehr, T. Petersen, M.B. Thomaidis, L.

Abstract

Background. The genetic diagnosis of mental retardation (MR) is difficult to establish and at present many cases remain undiagnosed and unexplained. Standard karyotyping has been used as one of the routine techniques for the last decades. The implementation of Array Comparative Genomic Hybridization (array-CGH) has enabled the analysis of copy number variants (CNVs) with high resolution. Major cohort studies attribute 11% of patients with unexplained mental retardation to clinically significant CNVs. Here we report the use of array-CGH for the first time in a Greek cohort. A total of 82 children of Greek origin with mean age 4.9 years were analysed in the present study. Patients with visible cytogenetic abnormalities ascertained by standard karyotyping as well as those with subtelomeric abnormalities determined by Multiplex Ligation-dependent Probe Amplification (MLPA) or subtelomeric FISH had been excluded. Results. Fourteen CNVs were detected in the studied patients. In nine patients (11%) the chromosomal aberrations were inherited from one of the parents. One patients showed two duplications, a 550 kb duplication in 3p14.1 inherited from the father and a ∼1.1 Mb duplication in (22)(q13.1q13.2) inherited from the mother. Although both parents were phenotypically normal, it cannot be excluded that the dual duplication is causative for the patient's clinical profile including dysmorphic features and severe developmental delay. Furthermore, three de novo clinically significant CNVs were detected (3.7%). There was a ∼6 Mb triplication of 18q21.1 in a girl 5 years of age with moderate MR and mild dysmorphic features and a ∼4.8 Mb duplication at (10)(q11.1q11.21) in a 2 years old boy with severe MR, multiple congenital anomalies, severe central hypotonia, and ataxia. Finally, in a 3 year-old girl with microcephaly and severe hypotonia a deletion in (2)(q31.2q31.3) of about ∼3.9 Mb was discovered. All CNVs were confirmed by Fluorescence in situ hybridization (FISH). For the remaining 9 patients the detected CNVs (inherited duplications or deletions of 80 kb to 800 kb in size) were probably not associated with the clinical findings. Conclusions. Genomic microarrays have within the recent years proven to be a highly useful tool in the investigation of unexplained MR. The cohorts reported so far agree on an around 11% diagnostic yield of clinically significant CNVs in patients with unexplained MR. Various publicly available databases have been created for the interpretation of identified CNVs and parents are analyzed in case a rare CNV is identified in the child. We have conducted a study of Greek patients with unexplained MR and confirmed the high diagnostic value of the previous studies. It is important that the technique becomes available also in less developed countries when the cost of consumables will be reduced. © 2010 Manolakos et al; licensee BioMed Central Ltd.

Published
2010

40. Primary open angle glaucoma due to T377M MYOC: Population mapping of a Greek founder mutation in Northwestern Greece

Author

Kitsos, G., Petrou, Z., Grigoriadou, M., Samples, J. R., Hewitt, A. W., Kokotas, H., Giannoulia-Karantana, A., Mackey, D. A., Wirtz, M. K., Moschou, M., Ioannidis, J. P., and Petersen, M. B.

Abstract

BACKGROUND: Mutations in the MYOC gene have been shown to explain 5% of unrelated primary open angle glaucoma (POAG) in different populations. In particular, the T377M MYOC mutation has arisen at least three separate times in history, in Great Britain, India, and Greece. The purpose of this study is to investigate the distribution of the mutation among different population groups in the northwestern region of Greece. MATERIALS AND METHODS: We explored the distribution of the "Greek" T377M founder mutation in the Epirus region in Northwestern Greece, which could be its origin. Genotyping was performed in POAG cases and controls by PCR amplification of the MYOC gene, followed by digestion with restriction enzyme. Statistical analyses were performed by an exact test, the Kaplan-Meier method and the t-test. RESULTS: In the isolated Chrysovitsa village in the Pindus Mountains, a large POAG family demonstrated the T377M mutation in 20 of 66 family members while no controls from the Epirus region (n = 124) carried this mutation (P < 0.001). Among other POAG cases from Epirus, 2 out of 14 familial cases and 1 out of 80 sporadic cases showed the mutation (P = 0.057). The probability of POAG diagnosis with advancing age among mutation carriers was 23% at age 40, and reached 100% at age 75. POAG patients with the T377M mutation were diagnosed at a mean age of 51 years (SD +/- 13.9), which is younger than the sporadic or familial POAG cases: 63.1 (SD +/- 11) and 66.8 (SD +/- 9.8) years, respectively. CONCLUSIONS: The T377M mutation was found in high proportion in members of the Chrysovitsa family (30.3%), in lower proportion in familial POAG cases (14.2%) and seems rare in sporadic POAG cases (1.2%), while no controls (0%) from the Epirus region carried the mutation. Historical and geographical data may explain the distribution of this mutation within Greece and worldwide. Clin Ophthalmol

Published
2010

41. Glaucomatous type abnormalities in patients with systemic sclerosis

Author

Kitsos, G., Tsifetaki, N., Gorezis, S., and Drosos, A. A.

Subjects
Adult, Male, Glaucoma/diagnosis/*etiology/pathology, Optic Nerve/pathology/physiopathology, Eye/pathology/physiopathology, Case-Control Studies, Scleroderma, Systemic/*complications, Humans, Female, Middle Aged, Aged
Abstract

Clin Exp Rheumatol

Published
2007

42. A large GLC1C Greek family with a myocilin T377M mutation: inheritance and phenotypic variability

Author

Petersen, M. B., Kitsos, G., Samples, J. R., Gaudette, N. D., Economou-Petersen, E., Sykes, R., Rust, K., Grigoriadou, M., Aperis, G., Choi, D., Psilas, K., Craig, J. E., Kramer, P. L., Mackey, D. A., and Wirtz, M. K.

Subjects
Adult, Aged, 80 and over, Glaucoma, Open-Angle/ethnology/*genetics, Male, Genotype, DNA Mutational Analysis, Inheritance Patterns, Heteroduplex Analysis, Mutation, Middle Aged, Polymerase Chain Reaction, Chromosomes, Human, Pair 3/*genetics, Pedigree, Chromosomes, Human, Pair 1/*genetics, Phenotype, Haplotypes, Eye Proteins/*genetics, Exons/genetics, Humans, Female, Glycoproteins/*genetics, Greece/ethnology, Cytoskeletal Proteins/*genetics, Chromatography, High Pressure Liquid, Aged
Abstract

PURPOSE: POAG is a complex disease; therefore, families in which a glaucoma gene has been mapped may carry additional POAG genes. The goal of this study was to determine whether mutations in the myocilin (MYOC) gene on chromosome 1 are present in two POAG families, which have previously been mapped to the GLC1C locus on chromosome 3. METHODS: The three exons of MYOC were screened by denaturing (d)HPLC. Samples with heteroduplex peaks were sequenced. Clinical findings were compared with genotype status in all available family members over the age of 20 years. RESULTS: A T377M coding sequence change in MYOC was identified in family members of the Greek GLC1C family but not in the Oregon GLC1C family. Individuals carrying both the MYOC T377M variant and the GLC1C haplotype were more severely affected at an earlier age than individuals with just one of the POAG genes, suggesting that these two genes interact or that both contribute to the POAG phenotype in a cumulative way. Invest Ophthalmol Vis Sci

Published
2006

43. Refining the primary open-angle glaucoma GLC1C region on chromosome 3 by haplotype analysis

Author

Samples, J. R., Kitsos, G., Economou-Petersen, E., Steinkamp, P., Sykes, R., Rust, K., Patzer, C., Grigoriadou, M., Aperis, G., Psilas, K., Petersen, M. B., and Wirtz, M. K.

Subjects
Male, Glaucoma, Open-Angle/*genetics, Greece, Chromosome Mapping, Humans, Female, DNA/analysis, Haplotypes, Middle Aged, Chromosomes, Human, Pair 3/*genetics, United States, Microsatellite Repeats, Pedigree
Abstract

The GLC1C locus for primary open-angle glaucoma (POAG) is inherited as an autosomal dominant trait. This region on chromosome 3 is 11 cM long. DNA samples from members of a Greek and an American GLC1C family were obtained to determine whether additional typing of microsatellite markers in family members might narrow the region. GLC1C family members were evaluated clinically for POAG on the basis of open angles, intraocular pressures, cupping of discs, and visual fields. DNA samples from the Greek and Oregon GLC1C families were used to further refine the GLC1C region using microsatellite markers. A total of 22 affected members were identified in the two families. Common alleles for D3S3637 and D3S3612 were present in the disease haplotype from both families, suggesting that they may have a common founder. A newly diagnosed patient in the American family had a recombination in the distal portion of the GLC1C haplotype. This recombination narrows the GLC1C region from 11 to 4 cM. Clin Genet

Published
2004

44. Internet-based counselling of remote ophthalmological patients

Author

Labiris, G., Petounis, A., Kitsos, G., Aspiotis, M., and Psillas, K.

Subjects
Adult, Male, Eye Diseases/diagnosis/therapy, Remote Consultation/*statistics & numerical data, Middle Aged, Patient Acceptance of Health Care, Internet/*utilization, Patient Education as Topic, Patient Satisfaction, Humans, Female, Health Services Research, Ophthalmology/*statistics & numerical data, Aged
Abstract

Acta Ophthalmol Scand

Published
2003

45. Retinopathy of prematurity and other ocular problems in premature infants weighing less than 1500 g at birth

Author

Asproudis, I. C., Andronikou, S. K., Hotoura, E. A., Kalogeropoulos, C. D., Kitsos, G. K., and Psilas, K. E.

Subjects
Infant, Premature, Strabismus/*epidemiology, Incidence, Refractive Errors/*epidemiology, Infant, Newborn, Greece/epidemiology, Gestational Age, Cryosurgery, Optic Atrophy/*epidemiology, Retinal Hemorrhage/*epidemiology/surgery, Infant, Very Low Birth Weight, Retinopathy of Prematurity/*epidemiology/surgery, Humans, Retrospective Studies
Abstract

PURPOSE: To estimate the incidence of retinopathy of prematurity and other ocular problems in a population of preterm infants. METHODS: This retrospective study included all infants with gestational age (GA)

Published
2002

46. Our experience with perfluorohexyloctane (F6H8) as a temporary endotamponade in vitreoretinal surgery

Author

Stefaniotou, M. I., Aspiotis, M. V., Kitsos, G. D., Kalogeropoulos, C. D., Asproudis, I. C., and Psilas, K. G.

Subjects
Male, Retinal Perforations/*drug therapy, Treatment Outcome, Retinal Detachment/*drug therapy, Vitrectomy, Visual Acuity, Humans, Female, Middle Aged, Fluorocarbons/*therapeutic use, Intraocular Pressure, Aged, Epiretinal Membrane/surgery
Abstract

PURPOSE: To evaluate the use of F6H8 as a temporary endotamponade for complicated and special cases of retinal detachment instead of silicone oil. METHODS: We have used F6H8 with 14 patients since February 1999. Eight suffered from rhegmatogenous retinal detachment (RRD) with multiple tears located inferiorly. Three presented inferior traction retinal detachment (TRD) under silicone oil, two suffered from ocular trauma with inferior TRD, and one had idiopathic macular hole. The substance was introduced into the eye after pars plana vitrectomy and membrane peeling if needed, and we tried to introduce as much as possible. RESULTS: With F6H8 the retina was easily reattached in all cases, like with perfluorocarbon liquids. The postoperative view was very good. F6H8 was removed in all cases after 3-8 weeks. Anatomical success was achieved in 12 out of 14 eyes. Two eyes presented severe PVR. F6H8 entered the anterior chamber in 4 cases, but no corneal complications occurred. In one case there was a marked IOP rise due to an anterior block, treated with superior iridotomy. In two cases retinal detachment (RD) occurred in the upper part and was treated with additional surgery, F6H8 removal and silicone oil injection. CONCLUSIONS: F6H8 seems to be a promising tamponade agent for special cases of RD. Eur J Ophthalmol

Published
2002

47. Primary open angle glaucoma due to T377M MYOC: Population mapping of a Greek founder mutation in Northwestern Greece

Author

Kitsos, G, Petrou, Z, Grigoriadou, M, Samples, JR, Hewitt, AW, Kokotas, H, Giannoulia-Karantana, A, Mackey, DA, Wirtz, MK, Moschou, M, Ioannidis, JP, Petersen, MB, Kitsos, G, Petrou, Z, Grigoriadou, M, Samples, JR, Hewitt, AW, Kokotas, H, Giannoulia-Karantana, A, Mackey, DA, Wirtz, MK, Moschou, M, Ioannidis, JP, and Petersen, MB

Abstract

BACKGROUND: Mutations in the MYOC gene have been shown to explain 5% of unrelated primary open angle glaucoma (POAG) in different populations. In particular, the T377M MYOC mutation has arisen at least three separate times in history, in Great Britain, India, and Greece. The purpose of this study is to investigate the distribution of the mutation among different population groups in the northwestern region of Greece. MATERIALS AND METHODS: We explored the distribution of the "Greek" T377M founder mutation in the Epirus region in Northwestern Greece, which could be its origin. Genotyping was performed in POAG cases and controls by PCR amplification of the MYOC gene, followed by digestion with restriction enzyme. Statistical analyses were performed by an exact test, the Kaplan-Meier method and the t-test. RESULTS: In the isolated Chrysovitsa village in the Pindus Mountains, a large POAG family demonstrated the T377M mutation in 20 of 66 family members while no controls from the Epirus region (n = 124) carried this mutation (P < 0.001). Among other POAG cases from Epirus, 2 out of 14 familial cases and 1 out of 80 sporadic cases showed the mutation (P = 0.057). The probability of POAG diagnosis with advancing age among mutation carriers was 23% at age 40, and reached 100% at age 75. POAG patients with the T377M mutation were diagnosed at a mean age of 51 years (SD +/- 13.9), which is younger than the sporadic or familial POAG cases: 63.1 (SD +/- 11) and 66.8 (SD +/- 9.8) years, respectively. CONCLUSIONS: The T377M mutation was found in high proportion in members of the Chrysovitsa family (30.3%), in lower proportion in familial POAG cases (14.2%) and seems rare in sporadic POAG cases (1.2%), while no controls (0%) from the Epirus region carried the mutation. Historical and geographical data may explain the distribution of this mutation within Greece and worldwide.

Published
2010

48. Copper and zinc serum levels in Stargardt's disease and retinitis pigmentosa

Author

Psilas, K., Kalfakakou, V., Kalogeropoulos, C., Kitsos, G., Zoumpouli, E., Aspiotis, M., and Galani, A.

Subjects
macular degeneration, dystrophy, copper, retinitis pigmentosa, fundus-flavimaculatus, zinc, trace elements, deficiency, rds gene, stargardt's disease, taurine, metabolism, retinal dysfunction
Abstract

Copper (Cu) and zinc (Zn) are essential trace elements for the structure and function of the retina, particularly for the pigment epithelium and photoreceptors, where they participate as coenzymes in very important reactions. This study was to determine whether patients with Stargardt's disease and with typical retinitis pigmentosa show changes in serum levels for Cu and Zn, Serum analysis for Cu and Zn concentrations was performed by means of a Perkin Elmer 560 atomic absorption spectrophotometer, in 10 patients with retinitis pigmentosa (group RP), 10 patients with Stargardt's disease (group St) and 10 normal individuals (group N) of the same age range, all were inhabitants of the same region. Statistical analysis of the results was carried out using the Student's t test. The mean serum levels (+/- SD) of Zn (mu g/ml) in groups RP, St, aad N were 0.51 +/- 0.1, 0.79 +/- 0.1, and 0.98 +/- 0.15, respectively. The mean serum levels (+/- SD) of Cu (mu g/ml) in groups RP, St, and N were 1.04 +/- 0.2, 0.95 +/- 0.14, and 0.94 +/- 0.1, respectively, Zinc serum levels were found to be significantly lower (p < 0.001) in retinitis pigmentosa and Stargardt's disease (p = 0.003) compared to those of normal subjects. In addition, zinc serum levels were significantly lower (p < 0.001) in patients with retinitis pigmentosa compared to those with Stargardt's disease. Cu serum levels did not differ significantly between the groups. Our results suggest that these 2 retinal diseases are associated with disturbances mainly of zinc metabolism. Zn serum levels difference between Stargardt's disease and typical retinitis pigmentosa is probably related to the pathophysiology and type of lesions in these diseases. Trace Elements and Electrolytes

Published
1997

49. Partial trisomy 17q22-qter and partial monosomy Xq27-qter in a girl with a de novo unbalanced translocation due to a postzygotic error: Case report and review of the literature on partial trisomy 17qter

Author

Sarri, C Gyftodimou, J Avramopoulos, D Grigoriadou, M and Pedersen, W Pandelia, E Pangalos, C Abazis, D Kitsos, G and Vassilopoulos, D BrondumNielsen, K Petersen, MB

Abstract

Partial trisomy 17q22-qter is a rare but well-recognized clinical entity, We present a case of partial trisomy for the long arm of chromosome 17, which was detected in a female infant with severe psychomotor and somatic retardation, Stargardt disease, short limbs, and numerous minor anomalies. Differential chromosomal staining demonstrated an excess of genetic material on the long arm of the late replicating X chromosome, FISH and DNA polymorphism analysis showed that the extra material belonged to the distal part of the long arm of chromosome 17 and that there was a partial monosomy of the distal part of the long arm of the derivative X chromosome, The breakpoint regions of this translocation were identified by molecular analysis using polymorphic microsatellite markers on human chromosomes 17 and X The origin of the abnormal X chromosome was found to be paternal, whereas the origin of the duplicated part of chromosome 17 was maternal, The unbalanced translocation between the paternal X and the maternal chromosome 17 is, therefore, suggested to be due to a postzygotic error. (C) 1997 Wiley-Liss, Inc.

Published
1997

50. Exclusion of one pedigree affected by adult onset primary open angle glaucoma from linkage to the juvenile glaucoma locus on chromosome 1q21-q31

Author

Avramopoulos, D Kitsos, G EconomouPetersen, E Grigoriadou, M and Vassilopoulos, D Papageorgiou, C Psilas, K Petersen, MB

Subjects
genetic structures, sense organs, eye diseases
Abstract

A locus for autosomal dominant juvenile onset primary open angle glaucoma (POAG) was recently assigned to chromosome region 1q21-q31. In the present study, a large Greek family with autosomal dominant adult onset POAG was investigated using microsatellite markers. Exclusion of Linkage of the adult onset POAG gene to the region D1S194-D1S191 was obtained in this pedigree. Therefore, the data provide evidence that juvenile and adult onset POAG are genetically distinct disease entities.

Published
1996

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