Search

Your search keyword '"Pott, J.W.R."' showing total 17 results
Start Over Author "Pott, J.W.R."
17 results on '"Pott, J.W.R."'

3. Stargardt disease: monitoring incidence and diagnostic trends in the Netherlands using a nationwide disease registry

Author

Runhart, E.H., Dhooge, P.P.A., Meester-Smoor, M., Pas, J.A.A.H., Pott, J.W.R., Leeuwen, R. Van, Kroes, H.Y., Bergen, A.A., Jong-Hesse, Y. de, Thiadens, A.A.H.J., Schooneveld, M.J. van, Genderen, M. van, Boon, C.J.F., Klaver, C.C.W., Born, L.I. van den, Cremers, F.P.M., Hoyng, C.B., Runhart, E.H., Dhooge, P.P.A., Meester-Smoor, M., Pas, J.A.A.H., Pott, J.W.R., Leeuwen, R. Van, Kroes, H.Y., Bergen, A.A., Jong-Hesse, Y. de, Thiadens, A.A.H.J., Schooneveld, M.J. van, Genderen, M. van, Boon, C.J.F., Klaver, C.C.W., Born, L.I. van den, Cremers, F.P.M., and Hoyng, C.B.

Abstract

Contains fulltext : 251561.pdf (Publisher’s version ) (Open Access), PURPOSE: To assess the incidence of Stargardt disease (STGD1) and to evaluate demographics of incident cases. METHODS: For this retrospective cohort study, demographic, clinical and genetic data of patients with a clinical diagnosis of STGD1 were registered between September 2010 and January 2020 in a nationwide disease registry. Annual incidence (2014-2018) and point prevalence (2018) were assessed on the basis of this registry. RESULTS: A total of 800 patients were registered, 56% were female and 83% were of European ancestry. The incidence was 1.67-1.95:1,000,000 per year and the point prevalence in 2018 was approximately 1:22,000-1:19,000 (with and without 10% of potentially unregistered cases). Age at onset was associated with sex (p = 0.027, Fisher's exact); 1.9x more women than men were observed (140 versus 74) amongst patients with an age at onset between 10 and 19 years, while the sex ratio in other age-at-onset categories approximated one. Late-onset STGD1 (≥45 years) constituted 33% of the diagnoses in 2014-2018 compared to 19% in 2004-2008. Diagnostic delay (≥2 years between the first documentation of macular abnormalities and diagnosis) was associated with older age of onset (p = 0.001, Mann-Whitney). Misdiagnosis for age-related macular degeneration (22%) and incidental STGD1 findings (14%) was common in patients with late-onset STGD1. CONCLUSION: The observed prevalence of STGD1 in real-world data was lower than expected on the basis of population ABCA4 allele frequencies. Late-onset STGD1 was more frequently diagnosed in recent years, likely due to higher awareness of its phenotype. In this pretherapeutic era, mis- and underdiagnosis of especially late-onset STGD1 and the role of sex in STGD1 should receive special attention.

Published
2022

5. LONGITUDINAL STUDY OF RPE65-ASSOCIATED INHERITED RETINAL DEGENERATIONS

Author

Pierrache, L.H.M., Ghafaryasl, B., Khan, M.I., Yzer, S., Genderen, M.M. van, Schuil, J., Boonstra, F.N., Pott, J.W.R., Faber, J., Tjon-Fo-Sang, M.J.H., Vermeer, K.A., Cremers, F.P.M., Klaver, C.C.W., Born, L.I. van den, Pierrache, L.H.M., Ghafaryasl, B., Khan, M.I., Yzer, S., Genderen, M.M. van, Schuil, J., Boonstra, F.N., Pott, J.W.R., Faber, J., Tjon-Fo-Sang, M.J.H., Vermeer, K.A., Cremers, F.P.M., Klaver, C.C.W., and Born, L.I. van den

Abstract

Contains fulltext : 225467.pdf (Publisher’s version ) (Closed access), PURPOSE: To study the disease course of RPE65-associated inherited retinal degenerations (IRDs) as a function of the genotype, define a critical age for blindness, and identify potential modifiers. METHODS: Forty-five patients with IRD from 33 families with biallelic RPE65 mutations, 28 stemming from a genetic isolate. We collected retrospective data from medical charts. Coexisting variants in 108 IRD-associated genes were identified with Molecular Inversion Probe analysis. RESULTS: Most patients were diagnosed within the first years of life. Daytime visual function ranged from near-normal to blindness in the first four decades and met WHO criteria for blindness for visual acuity and visual field in the fifth decade. p.(Thr368His) was the most common variant (54%). Intrafamilial variability and interfamilial variability in disease severity and progression were observed. Molecular Inversion Probe analysis confirmed all RPE65 variants and identified one additional variant in LRAT and one in EYS in two separate patients. CONCLUSION: All patients with RPE65-associated IRDs developed symptoms within the first year of life. Visual function in childhood and adolescence varied but deteriorated inevitably toward blindness after age 40. In this study, genotype was not predictive of clinical course. The variance in severity of disease could not be explained by double hits in other IRD genes.

Published
2020

6. LONGITUDINAL STUDY OF RPE65-ASSOCIATED INHERITED RETINAL DEGENERATIONS

Author

Pierrache, L. (Laurence), Ghafaryasl, B. (Babak), Khan, M.I. (Muhammad), Yzer, S. (Suzanne), van Genderen, M.M. (Maria M.), Schuil, J. (Jose), Boonstra, F.N. (F Nienke), Pott, J.W.R., Faber, J.T.H.N. de, Tjon-Fo-Sang, M.J. (Martha), Vermeer, K.A. (Koen), Cremers, F.P.M. (Frans), Klaver, C.C.W. (Caroline), Born, L.I. (Ingeborgh) van den, Pierrache, L. (Laurence), Ghafaryasl, B. (Babak), Khan, M.I. (Muhammad), Yzer, S. (Suzanne), van Genderen, M.M. (Maria M.), Schuil, J. (Jose), Boonstra, F.N. (F Nienke), Pott, J.W.R., Faber, J.T.H.N. de, Tjon-Fo-Sang, M.J. (Martha), Vermeer, K.A. (Koen), Cremers, F.P.M. (Frans), Klaver, C.C.W. (Caroline), and Born, L.I. (Ingeborgh) van den

Abstract

PURPOSE: To study the disease course of RPE65-associated inherited retinal degenerations (IRDs) as a function of the genotype, define a critical age for blindness, and identify potential modifiers. METHODS: Forty-five patients with IRD from 33 families with biallelic RPE65 mutations, 28 stemming from a genetic isolate. We collected retrospective data from medical charts. Coexisting variants in 108 IRD-associated genes were identified with Molecular Inversion Probe analysis. RESULTS: Most patients were diagnosed within the first years of life. Daytime visual function ranged from near-normal to blindness in the first four decades and met WHO criteria for blindness for visual acuity and visual field in the fifth decade. p.(Thr368His) was the most common variant (54%). Intrafamilial variability and interfamilial variability in disease severity and progression were observed. Molecular Inversion Probe analysis confirmed all RPE65 variants and identified one additional variant in LRAT and one in EYS in two separate patients. CONCLUSION: All patients with RPE65-associated IRDs developed symptoms within the first year of life. Visual function in childhood and adolescence varied but deteriorated inevitably toward blindness after age 40. In this study, genotype was not predictive of clinical course. The variance in severity of disease could not be explained by double hits in other IRD genes.

Published
2020
Full Text
View/download PDF

7. Cyclic esotropia and the treatment of over-elevation in adduction and V-pattern

Author

Pott, J.W.R., Godts, D., Kerkhof, D.B., and de Faber, J.T.H.N.

Subjects
Convergent strabismus -- Research, Health, Research
Abstract

Br J Ophthalmol 2004;88:66-68 Aim: To describe the development and treatment of V-pattern and bilateral over-elevation in adduction in patients with cyclic esotropia. Methods: Three patients with cyclic esotropia are [...]

Published
2004

8. Deep-intronic ABCA4 variants explain missing heritability in Stargardt disease and allow correction of splice defects by antisense oligonucleotides

Author

Sangermano, R, Garanto, A., Khan, M. (Mubeen), Runhart, E.H., Bauwens, M., Bax, N.M.A. (Klaas), Born, L.I. (Ingeborgh) van den, Khan, M.I. (Muhammad), Cornelis, S.S., Verheij, J, Pott, J.W.R., Thiadens, A., Klaver, C.C.W. (Caroline), Puech, B., Meunier, I., Naessens, S., Arno, G., Fakin, A., Carss, K.J., Raymond, FL, Webster, A.R. (Andrew), Dhaenens, C.M., Stohr, H., Grassmann, F. (Felix), Weber, B.H.F. (Bernhard), Hoyng, C.B. (Carel), De Baere, E. (Elfride), Albert, S., Collin, R.W.J. (Rob), Cremers, F.P.M. (Frans), Sangermano, R, Garanto, A., Khan, M. (Mubeen), Runhart, E.H., Bauwens, M., Bax, N.M.A. (Klaas), Born, L.I. (Ingeborgh) van den, Khan, M.I. (Muhammad), Cornelis, S.S., Verheij, J, Pott, J.W.R., Thiadens, A., Klaver, C.C.W. (Caroline), Puech, B., Meunier, I., Naessens, S., Arno, G., Fakin, A., Carss, K.J., Raymond, FL, Webster, A.R. (Andrew), Dhaenens, C.M., Stohr, H., Grassmann, F. (Felix), Weber, B.H.F. (Bernhard), Hoyng, C.B. (Carel), De Baere, E. (Elfride), Albert, S., Collin, R.W.J. (Rob), and Cremers, F.P.M. (Frans)

Abstract

Purpose: Using exome sequencing, the underlying variants in many persons with autosomal recessive diseases remain undetected. We explored autosomal recessive Stargardt disease (STGD1) as a model to identify the missing heritability. Methods: Sequencing of ABCA4 was performed in 8 STGD1 cases with one variant and p.Asn1868Ile in trans, 25 cases with one variant, and 3 cases with no ABCA4 variant. The effect of intronic variants was analyzed using in vitro splice assays in HEK293T cells and patient-derived fibroblasts. Antisense oligonucleotides were used to correct splice defects. Results: In 24 of the probands (67%), one known and five novel deep-intronic variants were found. The five novel variants resulted in messenger RNA pseudoexon inclusions, due to strengthening of cryptic splice sites or by disrupting a splicing silencer motif. Variant c.769-784C>T showed partial insertion of a pseudoexon and was found in cis with c.5603A>T (p.Asn1868Ile), so its causal role could not be fully established. Variant c.4253+43G>A resulted in partial skipping of exon 28. Remarkably, antisense oligonucleotides targeting the aberrant splice processes resulted in (partial) correction of all splicing defects. Conclusion: Our data demonstrate the importance of assessing noncoding variants in genetic diseases, and show the great potential of splice modulation therapy for deep-intronic variants.

Published
2019
Full Text
View/download PDF

9. Diagnostic exome sequencing in 266 Dutch patients with visual impairment

Author

Haer-Wigman, L. (Lonneke), Zelst-Stams, W.A. van, Pfundt, R. (Rolph), Born, L.I. (Ingeborgh) van den, Klaver, C.C.W. (Caroline), Verheij, J.B. (Joke), Hoyng, C.B. (Carel), Breuning, M.H. (Martijn), Boon, C.J.F. (Camiel), Kievit, A.J.A. (Anneke J.A.), Verhoeven, V.J.M. (Virginie), Pott, J.W.R., Sallevelt, S.C.E.H. (Suzanne), Hagen, J.M. (Johanna) van, Plomp, A. (Astrid), Kroes, H.Y. (Hester), Lelieveld, S.H. (Stefan H.), Hehir-Kwa, J. (Jayne), Castelein, S. (Steven), Nelen, M.R. (Marcel), Scheffer, H. (Hans), Lugtenberg, D. (Dorien), Cremers, F.P.M. (Frans), Hoefsloot, E.H. (Lies), Yntema, H.G., Haer-Wigman, L. (Lonneke), Zelst-Stams, W.A. van, Pfundt, R. (Rolph), Born, L.I. (Ingeborgh) van den, Klaver, C.C.W. (Caroline), Verheij, J.B. (Joke), Hoyng, C.B. (Carel), Breuning, M.H. (Martijn), Boon, C.J.F. (Camiel), Kievit, A.J.A. (Anneke J.A.), Verhoeven, V.J.M. (Virginie), Pott, J.W.R., Sallevelt, S.C.E.H. (Suzanne), Hagen, J.M. (Johanna) van, Plomp, A. (Astrid), Kroes, H.Y. (Hester), Lelieveld, S.H. (Stefan H.), Hehir-Kwa, J. (Jayne), Castelein, S. (Steven), Nelen, M.R. (Marcel), Scheffer, H. (Hans), Lugtenberg, D. (Dorien), Cremers, F.P.M. (Frans), Hoefsloot, E.H. (Lies), and Yntema, H.G.

Abstract

Inherited eye disorders have a large clinical and genetic heterogeneity, which makes genetic diagnosis cumbersome. An exome-sequencing approach was developed in which data analysis was divided into two steps: the vision gene panel and exome analysis. In the vision gene panel analysis, variants in genes known to cause inherited eye disorders were assessed for pathogenicity. If no causative variants were detected and when the patient consented, the entire exome data was analyzed. A total of 266 Dutch patients with different types of inherited eye disorders, including inherited retinal dystrophies, cataract, developmental eye disorders and optic atrophy, were investigated. In the vision gene panel analysis (likely), causative variants were detected in 49% and in the exome analysis in an additional 2% of the patients. The highest detection rate of (likely) causative variants was in patients with inherited retinal dystrophies, for instance a yield of 63% in patients with retinitis pigmentosa. In patients with developmental eye defects, cataract and optic atrophy, the detection rate was 50, 33 and 17%, respectively. An exome-sequencing approach enables a genetic diagnosis in patients with different types of inherited eye disorders using one test. The exome approach has the same detection rate as targeted panel sequencing tests, but offers a number of advantages. For instance, the vision gene panel can be frequently and easily updated with additional (novel) eye disorder genes. Determination of the genetic diagnosis improved the clinical diagnosis, regarding the assessment of the inheritance pattern as well as future disease perspective.

Published
2017
Full Text
View/download PDF

10. Development of Refractive Errors—What Can We Learn From Inherited Retinal Dystrophies?

Author

Hendriks, M. (Michelle), Verhoeven, V.J.M. (Virginie), Buitendijk, G.H.S. (Gabrielle), Polling, J.R. (Jan Roelof), Meester-Smoor, M.A. (Magda), Hofman, A. (Albert), van Huet, R.A.C. (Ramon A. C.), Klevering, B.J. (B. Jeroen), Bax, N.M. (Nathalie), Lambertus, S. (Stanley), Klaver, C.C.W. (Caroline C.W.), Hoyng, C.B. (Carel), Oomen, C.J. (Clasien J.), Zelst-Stams, W.A. van, Cremers, F.P.M. (Frans), Plomp, A. (Astrid), Schooneveld, M.J. (Mary), van Genderen, M.M. (Mies M.), Schuil, J. (Jose), Boonstra, F.N. (F. Nienke), Schlingemann, R.O. (Reinier), Bergen, A.A.B. (Arthur), Pierrache, L. (Laurence), Meester-Smoor, M. (Magda), Born, L.I. (Ingeborgh) van den, Boon, C.J.F. (Camiel), Pott, J.W.R., Leeuwen, R. (Redmer) van, Kroes, H.Y. (Hester), de Jong-Hesse, Y. (Yvonne), Kamermans, M. (Maarten), Klaver, C.C.W. (Caroline), Hendriks, M. (Michelle), Verhoeven, V.J.M. (Virginie), Buitendijk, G.H.S. (Gabrielle), Polling, J.R. (Jan Roelof), Meester-Smoor, M.A. (Magda), Hofman, A. (Albert), van Huet, R.A.C. (Ramon A. C.), Klevering, B.J. (B. Jeroen), Bax, N.M. (Nathalie), Lambertus, S. (Stanley), Klaver, C.C.W. (Caroline C.W.), Hoyng, C.B. (Carel), Oomen, C.J. (Clasien J.), Zelst-Stams, W.A. van, Cremers, F.P.M. (Frans), Plomp, A. (Astrid), Schooneveld, M.J. (Mary), van Genderen, M.M. (Mies M.), Schuil, J. (Jose), Boonstra, F.N. (F. Nienke), Schlingemann, R.O. (Reinier), Bergen, A.A.B. (Arthur), Pierrache, L. (Laurence), Meester-Smoor, M. (Magda), Born, L.I. (Ingeborgh) van den, Boon, C.J.F. (Camiel), Pott, J.W.R., Leeuwen, R. (Redmer) van, Kroes, H.Y. (Hester), de Jong-Hesse, Y. (Yvonne), Kamermans, M. (Maarten), and Klaver, C.C.W. (Caroline)

Abstract

Purpose It is unknown which retinal cells are involved in the retina-to-sclera signaling cascade causing myopia. As inherited retinal dystrophies (IRD) are characterized by dysfunction of a single retinal cell type and have a high risk of refractive errors, a study investigating the affected cell type, causal gene, and refractive error in IRDs may provide insight herein. Design Case-control study. Methods STUDY POPULATION: Total of 302 patients with IRD from 2 ophthalmogenetic centers in the Netherlands. REFERENCE POPULATION: Population-based Rotterdam Study-III and Erasmus Rucphen Family Study (N = 5550). Distributions and mean spherical equivalent (SE) were calculated for main affected cell type and causal gene; and risks of myopia and hyperopia were evaluated using logistic regression. Results Bipolar cell-related dystrophies were associated with the highest risk of SE high myopia 239.7; odds ratio (OR) mild hyperopia 263.2, both P <.0001; SE −6.86 diopters (D) (standard deviation [SD] 6.38), followed by cone-dominated dystrophies (OR high myopia 19.5, P <.0001; OR high hyperopia 10.7, P =.033; SE −3.10 D [SD 4.49]); rod dominated dystrophies (OR high myopia 10.1, P <.0001; OR high hyperopia 9.7, P =.001; SE −2.27 D [SD 4.65]), and retinal pigment epithelium (RPE)-related dystrophies (OR low myopia 2.7; P =.001; OR high hyperopia 5.8; P =.025; SE −0.10 D [SD 3.09]). Mutations in RPGR (SE −7.63 D [SD 3.31]) and CACNA1F (SE −5.33 D [SD 3.10]) coincided with the highest degree of myopia and in CABP4 (SE 4.81 D [SD 0.35]) with the highest degree of hyperopia. Conclusions Refractive errors, in particular myopia, are common in IRD. The bipolar synapse and the inner and outer segments of the photoreceptor may serve as critical sites for myopia development.

Published
2017
Full Text
View/download PDF

11. A novel nonsense mutation in CEP290 induces exon skipping and leads to a relatively mild retinal phenotype

Author

Littink, K.W. (Karin), Pott, J.W.R., Collin, R.W.J. (Rob), Kroes, H.Y. (Hester), Verheij, J.B. (Joke), Blokland, E.A.W. (Ellen), Miró, M.C., Hoyng, C.B. (Carel), Klaver, C.C.W. (Caroline), Koenekoop, R.K. (Robert), Rohrschneider, K. (Klaus), Cremers, F.P.M. (Frans), Born, L.I. (Ingeborgh) van den, Hollander, A.I. (Anneke), Littink, K.W. (Karin), Pott, J.W.R., Collin, R.W.J. (Rob), Kroes, H.Y. (Hester), Verheij, J.B. (Joke), Blokland, E.A.W. (Ellen), Miró, M.C., Hoyng, C.B. (Carel), Klaver, C.C.W. (Caroline), Koenekoop, R.K. (Robert), Rohrschneider, K. (Klaus), Cremers, F.P.M. (Frans), Born, L.I. (Ingeborgh) van den, and Hollander, A.I. (Anneke)

Abstract

Purpose. To identify the genetic defect in a family with variable retinal phenotypes. The proband had a diagnosis of Leber congenital amaurosis (LCA), whereas her two cousins had an early-onset severe retinal dystrophy (EOSRD) with useful vision. A distant family member had retinitis pigmentosa (RP). Methods. DNA samples of the affected family members were genotyped with 250 K genome-wide SNP microarrays. Genetic defects were localized by linkage analysis and homozygosity mapping, and candidate genes were analyzed by sequencing. Patients underwent a full ophthalmic examination. Results. Compound heterozygous mutations in CEP290 were identified in the proband and her two cousins: the frequent c.2991 + 1655A>G founder mutation and a novel nonsense mutation in exon 7 (c.451C>T, p.Arg151X). The proband had nystagmus, hyperopia, a flat electroretinogram (ERG), and decreased visual acuity (20/250) from birth. The two cousins had minimal scotopic ERG responses at the age of 2. In one of these patients, visual acuity had reached a level of 20/32 at age 5, which is high for patients with CEP290 mutations. Analysis of the CEP290 mRNA in affected individuals revealed altered splice forms in which either exon 7 or exons 7 and 8 were skipped. In both mutant cDNA products, the open reading frame was not disrupted. Furthermore, homozygosity mapping and mutation analysis in the distant family member affected by RP revealed a homozygous mutation in MERTK, but no CEP290 mutations. This MERTK mutation was heterozygously present in the most severely affected (LCA) patient, but was absent in the two more mildly affected cousins. Conclusions. A novel nonsense mutation in CEP290 results in nonsense-associated altered splicing. That the remaining open reading frame is intact may explain the less severe phenotype observed in the two affected cousins. The additional heterozygous mutation in MERTK may clarify the more severe pheno-type in the proband. This study extends the phenotypic spectru

Published
2010
Full Text
View/download PDF

13. Strabismus in very low birth weight and/or very preterm children: Discrepancy between age of onset and start of treatment

Author

Pott, J.W.R., Van Hof-van Duin, J. (J.), Heersema, D.J., Fetter, W.P.F. (Willem), Schreuder, A.M. (A.), Verloove-Vanhorick, S.P., Pott, J.W.R., Van Hof-van Duin, J. (J.), Heersema, D.J., Fetter, W.P.F. (Willem), Schreuder, A.M. (A.), and Verloove-Vanhorick, S.P.

Abstract

Present medical care is not sufficient for early detection and treatment of strabismus in at-risk children. Our results suggest that the optimal screening age for early detection of persistent strabismus in VLBW children is at 9 months of age. Because strabismus can also develop after this age, it is important to repeat examination of visual functions in at risk-children at regular intervals after 1 year of age.

Published
1995
Full Text
View/download PDF

14. Visuele functies bij 5-jarige kinderen in relatie tot een zeer laag geboortegewicht en/of een zeer korte zwangerschapsduur

Author

Pott, J.W.R. and Pott, J.W.R.

Abstract

Uit eerder onderzoek verricht op de afdeling Fysiologie I van de Erasmus Universiteit Rotterdam is gebleken dat kinderen, waarvan het geboortegewicht zeer laag was ( <1500 g, VLBW) een verhoogde kans hebben op stoornissen van de visuele ontwikkeling. Zeker 50% van de VLBW kinderen bleken in het eerste levensjaar afwijkingen te hebben in de ontwikkeling van de gezichtsscherpte, gezichtsvelden en/of binoculaire of monoculaire optokinetische nystagmus (OKN). Deze visuele stoornissen leken in verband te staan met perinataal cerebraal letsel. Het percentage VLBW kinderen met een visuele stoornis was het hoogst wanneer visueel onderzoek verricht werd op de leeftijd van 6 maanden. Na deze leeftijd (tussen de leeftijd van 6 maanden en 2 ½ jaar) bleek het percentage visueel gestoorde kinderen af te nemen. Deze resultaten wijzen erop dat de visuele ontwikkeling bij VLBW kinderen vertraagd kan verlopen. Anderzijds was het percentage visuele stoornissen op 2 ½-jarige leeftijd nog steed verhoogd. Het was onbekend of VLBW kinderen ook een verhoogde kans hebben op blijvende stoornissen van het zien. Om deze reden werden visuele functies onderzocht bij 450 5-jarige kinderen, waarvan het geboortegewicht minder dan 1500 gram was en/of de zwangerschapsduur korter dan 32 weken (in het huidige onderzoek risico kinderen genoemd). Ter vergelijking werden tevens 201 5-jarige controle kinderen onderzocht, waarvan het geboortegewicht tussen 2500 en 4500 gram was en de zwangerschapsduur tussen 37 en 42 weken.

Published
1992

17. Unilateral proptosis: the role of medical history.

Author

Kamminga, N., Jansonius, N.M., Pott, J.W.R., and Links, T.P.

Subjects
EXOPHTHALMOS, MEDICAL history taking, DIAGNOSIS
Abstract

Examines the role of medical history in the diagnosis of unilateral proptosis. Association between Graves' ophthalmopathy and Graves' hyperthyroidism; Antiparietal cell antibodies; Computed tomography.

Published
2003
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results