Your search keyword '"Lorenz, Birgit"' showing total 55 results

1. Twelve-month Natural History Study of Centrosomal Protein 290 (CEP290)-associated Inherited Retinal Degeneration

Author

Pierce, Eric A., Ashimatey, Bright S., Jayasundera, Thiran, Hoyng, C.B., Lam, B.L., Lorenz, Birgit, Myers, Rene, Pennesi, M.E., Pierce, Eric A., Ashimatey, Bright S., Jayasundera, Thiran, Hoyng, C.B., Lam, B.L., Lorenz, Birgit, Myers, Rene, and Pennesi, M.E.

Abstract

Contains fulltext : 307455.pdf (Publisher’s version ) (Open Access)

Published

2024

2. Comprehensive variant spectrum of the CNGA3 gene in patients affected by achromatopsia

Author

Solaki, Maria, Baumann, Britta, Reuter, Peggy, Andreasson, Sten, Audo, Isabelle, Ayuso, Carmen, Balousha, Ghassan, Benedicenti, Francesco, Birch, David, Bitoun, Pierre, Blain, Delphine, Bocquet, Beatrice, Branham, Kari, Català-Mora, Jaume, De Baere, Elfride, Dollfus, Helene, Falana, Mohammed, Giorda, Roberto, Golovleva, Irina, Gottlob, Irene, Heckenlively, John R., Jacobson, Samuel G., Jones, Kaylie, Jägle, Herbert, Janecke, Andreas R., Kellner, Ulrich, Liskova, Petra, Lorenz, Birgit, Martorell-Sampol, Loreto, Messias, André, Meunier, Isabelle, Belga Ottoni Porto, Fernanda, Papageorgiou, Eleni, Plomp, Astrid S., de Ravel, Thomy J. L., Reiff, Charlotte M., Renner, Agnes B., Rosenberg, Thomas, Rudolph, Günther, Salati, Roberto, Sener, E. Cumhur, Sieving, Paul A., Stanzial, Franco, Traboulsi, Elias I., Tsang, Stephen H., Varsanyi, Balázs, Weleber, Richard G., Zobor, Ditta, Stingl, Katarina, Wissinger, Bernd, Kohl, Susanne, Solaki, Maria, Baumann, Britta, Reuter, Peggy, Andreasson, Sten, Audo, Isabelle, Ayuso, Carmen, Balousha, Ghassan, Benedicenti, Francesco, Birch, David, Bitoun, Pierre, Blain, Delphine, Bocquet, Beatrice, Branham, Kari, Català-Mora, Jaume, De Baere, Elfride, Dollfus, Helene, Falana, Mohammed, Giorda, Roberto, Golovleva, Irina, Gottlob, Irene, Heckenlively, John R., Jacobson, Samuel G., Jones, Kaylie, Jägle, Herbert, Janecke, Andreas R., Kellner, Ulrich, Liskova, Petra, Lorenz, Birgit, Martorell-Sampol, Loreto, Messias, André, Meunier, Isabelle, Belga Ottoni Porto, Fernanda, Papageorgiou, Eleni, Plomp, Astrid S., de Ravel, Thomy J. L., Reiff, Charlotte M., Renner, Agnes B., Rosenberg, Thomas, Rudolph, Günther, Salati, Roberto, Sener, E. Cumhur, Sieving, Paul A., Stanzial, Franco, Traboulsi, Elias I., Tsang, Stephen H., Varsanyi, Balázs, Weleber, Richard G., Zobor, Ditta, Stingl, Katarina, Wissinger, Bernd, and Kohl, Susanne

Abstract

Achromatopsia (ACHM) is a congenital cone photoreceptor disorder characterized by impaired color discrimination, low visual acuity, photosensitivity, and nystagmus. To date, six genes have been associated with ACHM (CNGA3, CNGB3, GNAT2, PDE6C, PDE6H, and ATF6), the majority of these being implicated in the cone phototransduction cascade. CNGA3 encodes the CNGA3 subunit of the cyclic nucleotide-gated ion channel in cone photoreceptors and is one of the major disease-associated genes for ACHM. Herein, we provide a comprehensive overview of the CNGA3 variant spectrum in a cohort of 1060 genetically confirmed ACHM patients, 385 (36.3%) of these carrying “likely disease-causing” variants in CNGA3. Compiling our own genetic data with those reported in the literature and in public databases, we further extend the CNGA3 variant spectrum to a total of 316 variants, 244 of which we interpreted as “likely disease-causing” according to ACMG/AMP criteria. We report 48 novel “likely disease-causing” variants, 24 of which are missense substitutions underlining the predominant role of this mutation class in the CNGA3 variant spectrum. In addition, we provide extensive in silico analyses and summarize reported functional data of previously analyzed missense, nonsense and splicing variants to further advance the pathogenicity assessment of the identified variants.

Published

2022

3. Comprehensive variant spectrum of the CNGA3 gene in patients affected by achromatopsia

Author

Solaki, Maria, Baumann, Britta, Reuter, Peggy, Andreasson, Sten, Audo, Isabelle, Ayuso, Carmen, Balousha, Ghassan, Benedicenti, Francesco, Birch, David, Bitoun, Pierre, Blain, Delphine, Bocquet, Beatrice, Branham, Kari, Català-Mora, Jaume, De Baere, Elfride, Dollfus, Helene, Falana, Mohammed, Giorda, Roberto, Golovleva, Irina, Gottlob, Irene, Heckenlively, John R., Jacobson, Samuel G., Jones, Kaylie, Jägle, Herbert, Janecke, Andreas R., Kellner, Ulrich, Liskova, Petra, Lorenz, Birgit, Martorell-Sampol, Loreto, Messias, André, Meunier, Isabelle, Belga Ottoni Porto, Fernanda, Papageorgiou, Eleni, Plomp, Astrid S., de Ravel, Thomy J. L., Reiff, Charlotte M., Renner, Agnes B., Rosenberg, Thomas, Rudolph, Günther, Salati, Roberto, Sener, E. Cumhur, Sieving, Paul A., Stanzial, Franco, Traboulsi, Elias I., Tsang, Stephen H., Varsanyi, Balázs, Weleber, Richard G., Zobor, Ditta, Stingl, Katarina, Wissinger, Bernd, Kohl, Susanne, Solaki, Maria, Baumann, Britta, Reuter, Peggy, Andreasson, Sten, Audo, Isabelle, Ayuso, Carmen, Balousha, Ghassan, Benedicenti, Francesco, Birch, David, Bitoun, Pierre, Blain, Delphine, Bocquet, Beatrice, Branham, Kari, Català-Mora, Jaume, De Baere, Elfride, Dollfus, Helene, Falana, Mohammed, Giorda, Roberto, Golovleva, Irina, Gottlob, Irene, Heckenlively, John R., Jacobson, Samuel G., Jones, Kaylie, Jägle, Herbert, Janecke, Andreas R., Kellner, Ulrich, Liskova, Petra, Lorenz, Birgit, Martorell-Sampol, Loreto, Messias, André, Meunier, Isabelle, Belga Ottoni Porto, Fernanda, Papageorgiou, Eleni, Plomp, Astrid S., de Ravel, Thomy J. L., Reiff, Charlotte M., Renner, Agnes B., Rosenberg, Thomas, Rudolph, Günther, Salati, Roberto, Sener, E. Cumhur, Sieving, Paul A., Stanzial, Franco, Traboulsi, Elias I., Tsang, Stephen H., Varsanyi, Balázs, Weleber, Richard G., Zobor, Ditta, Stingl, Katarina, Wissinger, Bernd, and Kohl, Susanne

Abstract

Achromatopsia (ACHM) is a congenital cone photoreceptor disorder characterized by impaired color discrimination, low visual acuity, photosensitivity, and nystagmus. To date, six genes have been associated with ACHM (CNGA3, CNGB3, GNAT2, PDE6C, PDE6H, and ATF6), the majority of these being implicated in the cone phototransduction cascade. CNGA3 encodes the CNGA3 subunit of the cyclic nucleotide-gated ion channel in cone photoreceptors and is one of the major disease-associated genes for ACHM. Herein, we provide a comprehensive overview of the CNGA3 variant spectrum in a cohort of 1060 genetically confirmed ACHM patients, 385 (36.3%) of these carrying “likely disease-causing” variants in CNGA3. Compiling our own genetic data with those reported in the literature and in public databases, we further extend the CNGA3 variant spectrum to a total of 316 variants, 244 of which we interpreted as “likely disease-causing” according to ACMG/AMP criteria. We report 48 novel “likely disease-causing” variants, 24 of which are missense substitutions underlining the predominant role of this mutation class in the CNGA3 variant spectrum. In addition, we provide extensive in silico analyses and summarize reported functional data of previously analyzed missense, nonsense and splicing variants to further advance the pathogenicity assessment of the identified variants.

Published

2022

4. Comprehensive variant spectrum of the CNGA3 gene in patients affected by achromatopsia

Author

Solaki, Maria, Baumann, Britta, Reuter, Peggy, Andreasson, Sten, Audo, Isabelle, Ayuso, Carmen, Balousha, Ghassan, Benedicenti, Francesco, Birch, David, Bitoun, Pierre, Blain, Delphine, Bocquet, Beatrice, Branham, Kari, Català-Mora, Jaume, De Baere, Elfride, Dollfus, Helene, Falana, Mohammed, Giorda, Roberto, Golovleva, Irina, Gottlob, Irene, Heckenlively, John R., Jacobson, Samuel G., Jones, Kaylie, Jägle, Herbert, Janecke, Andreas R., Kellner, Ulrich, Liskova, Petra, Lorenz, Birgit, Martorell-Sampol, Loreto, Messias, André, Meunier, Isabelle, Belga Ottoni Porto, Fernanda, Papageorgiou, Eleni, Plomp, Astrid S., de Ravel, Thomy J. L., Reiff, Charlotte M., Renner, Agnes B., Rosenberg, Thomas, Rudolph, Günther, Salati, Roberto, Sener, E. Cumhur, Sieving, Paul A., Stanzial, Franco, Traboulsi, Elias I., Tsang, Stephen H., Varsanyi, Balázs, Weleber, Richard G., Zobor, Ditta, Stingl, Katarina, Wissinger, Bernd, Kohl, Susanne, Solaki, Maria, Baumann, Britta, Reuter, Peggy, Andreasson, Sten, Audo, Isabelle, Ayuso, Carmen, Balousha, Ghassan, Benedicenti, Francesco, Birch, David, Bitoun, Pierre, Blain, Delphine, Bocquet, Beatrice, Branham, Kari, Català-Mora, Jaume, De Baere, Elfride, Dollfus, Helene, Falana, Mohammed, Giorda, Roberto, Golovleva, Irina, Gottlob, Irene, Heckenlively, John R., Jacobson, Samuel G., Jones, Kaylie, Jägle, Herbert, Janecke, Andreas R., Kellner, Ulrich, Liskova, Petra, Lorenz, Birgit, Martorell-Sampol, Loreto, Messias, André, Meunier, Isabelle, Belga Ottoni Porto, Fernanda, Papageorgiou, Eleni, Plomp, Astrid S., de Ravel, Thomy J. L., Reiff, Charlotte M., Renner, Agnes B., Rosenberg, Thomas, Rudolph, Günther, Salati, Roberto, Sener, E. Cumhur, Sieving, Paul A., Stanzial, Franco, Traboulsi, Elias I., Tsang, Stephen H., Varsanyi, Balázs, Weleber, Richard G., Zobor, Ditta, Stingl, Katarina, Wissinger, Bernd, and Kohl, Susanne

Abstract

Achromatopsia (ACHM) is a congenital cone photoreceptor disorder characterized by impaired color discrimination, low visual acuity, photosensitivity, and nystagmus. To date, six genes have been associated with ACHM (CNGA3, CNGB3, GNAT2, PDE6C, PDE6H, and ATF6), the majority of these being implicated in the cone phototransduction cascade. CNGA3 encodes the CNGA3 subunit of the cyclic nucleotide-gated ion channel in cone photoreceptors and is one of the major disease-associated genes for ACHM. Herein, we provide a comprehensive overview of the CNGA3 variant spectrum in a cohort of 1060 genetically confirmed ACHM patients, 385 (36.3%) of these carrying “likely disease-causing” variants in CNGA3. Compiling our own genetic data with those reported in the literature and in public databases, we further extend the CNGA3 variant spectrum to a total of 316 variants, 244 of which we interpreted as “likely disease-causing” according to ACMG/AMP criteria. We report 48 novel “likely disease-causing” variants, 24 of which are missense substitutions underlining the predominant role of this mutation class in the CNGA3 variant spectrum. In addition, we provide extensive in silico analyses and summarize reported functional data of previously analyzed missense, nonsense and splicing variants to further advance the pathogenicity assessment of the identified variants.

Published

2022

5. Retinopathy of Prematurity Update on Classification, Screening, and Therapy

Author

Li, Jeany Q., Kellner, Ulrich, Lorenz, Birgit, Stahl, Andreas, Krohne, Tim U., Li, Jeany Q., Kellner, Ulrich, Lorenz, Birgit, Stahl, Andreas, and Krohne, Tim U.

Abstract

Retinopathy of prematurity (ROP) is a leading cause of preventable childhood blindness. This proliferative retinal vascular disease affects only prematurely born infants. Major risk factors include low gestational age and prolonged postnatal oxygen supplementation. ROP screening allows for timely identification of treatment-requiring infants and thus significantly reduces the risk of severe visual impairment and blindness from ROP. Current treatment options comprise retinal laser coagulation and intravitreal anti-vascular endothelial growth factor (VEGF) therapy. We provide a review of scientific data and current treatment recommendations, with special attention to the updated German guideline on ROP screening, the statement of the German ophthalmological societies on anti-VEGF therapy of ROP, and the new third edition of the International Classification of Retinopathy of Prematurity (ICROP3).

Published

2022

6. National guideline for ophthalmological screening of premature infants in Germany (S2k level, AWMF guidelines register no. 024/010, March 2020)

Author

Maier, Rolf F., Hummler, Helmut, Kellner, Ulrich, Krohne, Tim U., Lawrenz, Burkhard, Lorenz, Birgit, Mitschdoerfer, Barbara, Roll, Claudia, Stahl, Andreas, Maier, Rolf F., Hummler, Helmut, Kellner, Ulrich, Krohne, Tim U., Lawrenz, Burkhard, Lorenz, Birgit, Mitschdoerfer, Barbara, Roll, Claudia, and Stahl, Andreas

Published

2022

7. Retina, Vitreous Humor, Ocular Fundus Prenatal Retinopathy

Author

Li, Jeany Q., Kellner, Ulrich, Lorenz, Birgit, Stahl, Andreas, Krohne, Tim U., Li, Jeany Q., Kellner, Ulrich, Lorenz, Birgit, Stahl, Andreas, and Krohne, Tim U.

Abstract

Retinopathy of prematurity (ROP) is a leading cause of preventable childhood blindness. This proliferative retinal vascular disease affects only prematurely born infants. Major risk factors include low gestational age and prolonged postnatal oxygen supplementation. ROP screening allows for timely identification of treatment-requiring infants and thus significantly reduces the risk of severe visual impairment and blindness from ROP. Current treatment options comprise retinal laser coagulation and intravitreal anti-vascular endothelial growth factor (VEGF) therapy. We provide a review of scientific data and current treatment recommendations, with special attention to the updated German guideline on ROP screening, the statement of the German ophthalmological societies on anti-VEGF therapy of ROP, and the new third edition of the International Classification of Retinopathy of Prematurity (ICROP3).

Published

2022

8. Comprehensive variant spectrum of the CNGA3 gene in patients affected by achromatopsia

Author

Solaki, Maria, Baumann, Britta, Reuter, Peggy, Andreasson, Sten, Audo, Isabelle, Ayuso, Carmen, Balousha, Ghassan, Benedicenti, Francesco, Birch, David, Bitoun, Pierre, Blain, Delphine, Bocquet, Beatrice, Branham, Kari, Català-Mora, Jaume, De Baere, Elfride, Dollfus, Helene, Falana, Mohammed, Giorda, Roberto, Golovleva, Irina, Gottlob, Irene, Heckenlively, John R., Jacobson, Samuel G., Jones, Kaylie, Jägle, Herbert, Janecke, Andreas R., Kellner, Ulrich, Liskova, Petra, Lorenz, Birgit, Martorell-Sampol, Loreto, Messias, André, Meunier, Isabelle, Belga Ottoni Porto, Fernanda, Papageorgiou, Eleni, Plomp, Astrid S., de Ravel, Thomy J. L., Reiff, Charlotte M., Renner, Agnes B., Rosenberg, Thomas, Rudolph, Günther, Salati, Roberto, Sener, E. Cumhur, Sieving, Paul A., Stanzial, Franco, Traboulsi, Elias I., Tsang, Stephen H., Varsanyi, Balázs, Weleber, Richard G., Zobor, Ditta, Stingl, Katarina, Wissinger, Bernd, Kohl, Susanne, Solaki, Maria, Baumann, Britta, Reuter, Peggy, Andreasson, Sten, Audo, Isabelle, Ayuso, Carmen, Balousha, Ghassan, Benedicenti, Francesco, Birch, David, Bitoun, Pierre, Blain, Delphine, Bocquet, Beatrice, Branham, Kari, Català-Mora, Jaume, De Baere, Elfride, Dollfus, Helene, Falana, Mohammed, Giorda, Roberto, Golovleva, Irina, Gottlob, Irene, Heckenlively, John R., Jacobson, Samuel G., Jones, Kaylie, Jägle, Herbert, Janecke, Andreas R., Kellner, Ulrich, Liskova, Petra, Lorenz, Birgit, Martorell-Sampol, Loreto, Messias, André, Meunier, Isabelle, Belga Ottoni Porto, Fernanda, Papageorgiou, Eleni, Plomp, Astrid S., de Ravel, Thomy J. L., Reiff, Charlotte M., Renner, Agnes B., Rosenberg, Thomas, Rudolph, Günther, Salati, Roberto, Sener, E. Cumhur, Sieving, Paul A., Stanzial, Franco, Traboulsi, Elias I., Tsang, Stephen H., Varsanyi, Balázs, Weleber, Richard G., Zobor, Ditta, Stingl, Katarina, Wissinger, Bernd, and Kohl, Susanne

Abstract

Achromatopsia (ACHM) is a congenital cone photoreceptor disorder characterized by impaired color discrimination, low visual acuity, photosensitivity, and nystagmus. To date, six genes have been associated with ACHM (CNGA3, CNGB3, GNAT2, PDE6C, PDE6H, and ATF6), the majority of these being implicated in the cone phototransduction cascade. CNGA3 encodes the CNGA3 subunit of the cyclic nucleotide-gated ion channel in cone photoreceptors and is one of the major disease-associated genes for ACHM. Herein, we provide a comprehensive overview of the CNGA3 variant spectrum in a cohort of 1060 genetically confirmed ACHM patients, 385 (36.3%) of these carrying “likely disease-causing” variants in CNGA3. Compiling our own genetic data with those reported in the literature and in public databases, we further extend the CNGA3 variant spectrum to a total of 316 variants, 244 of which we interpreted as “likely disease-causing” according to ACMG/AMP criteria. We report 48 novel “likely disease-causing” variants, 24 of which are missense substitutions underlining the predominant role of this mutation class in the CNGA3 variant spectrum. In addition, we provide extensive in silico analyses and summarize reported functional data of previously analyzed missense, nonsense and splicing variants to further advance the pathogenicity assessment of the identified variants.

Published

2022

9. Comprehensive variant spectrum of the CNGA3 gene in patients affected by achromatopsia

Author

Solaki, Maria, Baumann, Britta, Reuter, Peggy, Andreasson, Sten, Audo, Isabelle, Ayuso, Carmen, Balousha, Ghassan, Benedicenti, Francesco, Birch, David, Bitoun, Pierre, Blain, Delphine, Bocquet, Beatrice, Branham, Kari, Català-Mora, Jaume, De Baere, Elfride, Dollfus, Helene, Falana, Mohammed, Giorda, Roberto, Golovleva, Irina, Gottlob, Irene, Heckenlively, John R., Jacobson, Samuel G., Jones, Kaylie, Jägle, Herbert, Janecke, Andreas R., Kellner, Ulrich, Liskova, Petra, Lorenz, Birgit, Martorell-Sampol, Loreto, Messias, André, Meunier, Isabelle, Belga Ottoni Porto, Fernanda, Papageorgiou, Eleni, Plomp, Astrid S., de Ravel, Thomy J. L., Reiff, Charlotte M., Renner, Agnes B., Rosenberg, Thomas, Rudolph, Günther, Salati, Roberto, Sener, E. Cumhur, Sieving, Paul A., Stanzial, Franco, Traboulsi, Elias I., Tsang, Stephen H., Varsanyi, Balázs, Weleber, Richard G., Zobor, Ditta, Stingl, Katarina, Wissinger, Bernd, Kohl, Susanne, Solaki, Maria, Baumann, Britta, Reuter, Peggy, Andreasson, Sten, Audo, Isabelle, Ayuso, Carmen, Balousha, Ghassan, Benedicenti, Francesco, Birch, David, Bitoun, Pierre, Blain, Delphine, Bocquet, Beatrice, Branham, Kari, Català-Mora, Jaume, De Baere, Elfride, Dollfus, Helene, Falana, Mohammed, Giorda, Roberto, Golovleva, Irina, Gottlob, Irene, Heckenlively, John R., Jacobson, Samuel G., Jones, Kaylie, Jägle, Herbert, Janecke, Andreas R., Kellner, Ulrich, Liskova, Petra, Lorenz, Birgit, Martorell-Sampol, Loreto, Messias, André, Meunier, Isabelle, Belga Ottoni Porto, Fernanda, Papageorgiou, Eleni, Plomp, Astrid S., de Ravel, Thomy J. L., Reiff, Charlotte M., Renner, Agnes B., Rosenberg, Thomas, Rudolph, Günther, Salati, Roberto, Sener, E. Cumhur, Sieving, Paul A., Stanzial, Franco, Traboulsi, Elias I., Tsang, Stephen H., Varsanyi, Balázs, Weleber, Richard G., Zobor, Ditta, Stingl, Katarina, Wissinger, Bernd, and Kohl, Susanne

Abstract

Achromatopsia (ACHM) is a congenital cone photoreceptor disorder characterized by impaired color discrimination, low visual acuity, photosensitivity, and nystagmus. To date, six genes have been associated with ACHM (CNGA3, CNGB3, GNAT2, PDE6C, PDE6H, and ATF6), the majority of these being implicated in the cone phototransduction cascade. CNGA3 encodes the CNGA3 subunit of the cyclic nucleotide-gated ion channel in cone photoreceptors and is one of the major disease-associated genes for ACHM. Herein, we provide a comprehensive overview of the CNGA3 variant spectrum in a cohort of 1060 genetically confirmed ACHM patients, 385 (36.3%) of these carrying “likely disease-causing” variants in CNGA3. Compiling our own genetic data with those reported in the literature and in public databases, we further extend the CNGA3 variant spectrum to a total of 316 variants, 244 of which we interpreted as “likely disease-causing” according to ACMG/AMP criteria. We report 48 novel “likely disease-causing” variants, 24 of which are missense substitutions underlining the predominant role of this mutation class in the CNGA3 variant spectrum. In addition, we provide extensive in silico analyses and summarize reported functional data of previously analyzed missense, nonsense and splicing variants to further advance the pathogenicity assessment of the identified variants.

Published

2022

10. Yokoyama procedure for esotropia associated with high myopia: real-world data from a large-scale multicentre analysis

Author

Wabbels, Bettina, Fricke, Julia, Schittkowski, Michael, Graf, Michael, Lorenz, Birgit, Bau, Viktoria, Nentwich, Martin M., Atili, Abed, Eckstein, Anja, Sturm, Veit, Beisse, Christina, Sterker, Ina, Neppert, Birte, Mauschitz, Matthias M., Wabbels, Bettina, Fricke, Julia, Schittkowski, Michael, Graf, Michael, Lorenz, Birgit, Bau, Viktoria, Nentwich, Martin M., Atili, Abed, Eckstein, Anja, Sturm, Veit, Beisse, Christina, Sterker, Ina, Neppert, Birte, and Mauschitz, Matthias M.

Abstract

Purpose High myopic patients may develop strabismus due to globe dislocation out of the normal extraocular muscle cone. Surgical correction of this strabismus type is possible by joining the superior and lateral rectus muscles without the need for a scleral suture called the Yokoyama procedure. Data from large patient samples and the evaluation of a potential effect of an additional medial rectus recession (MRR) have been lacking so far. Methods We pooled retrospective patient data of 14 departments of ophthalmology in Germany and Switzerland and analysed determinants of postoperative results using multivariable regression models. Results We included 133 patients (mean age: 59.7 +/- 13.4 years, surgery between 2008 and 2017) with a mean preoperative esotropia (both Yokoyama with and without MRR) of 23.8 degrees +/- 4.6 degrees. The angle of preoperative esotropia increased with age. The postoperative esotropia was 8.7 degrees +/- 9.9 degrees, and six patients were overcorrected. While preoperative esotropia was highly associated with postoperative results, we found no association of additional MRR with any of our postoperative outcome measures. The Yokoyama procedure had a higher absolute effect in patients with higher preoperative esotropia. Conclusion Our study confirms the positive effect of the Yokoyama procedure on strabismus due to high myopia in large-scale real-world data. In some cases, MRR may be needed because of muscle contracture, although additional MRR statistically did not affect the postoperative outcome. In patients with bilateral high myopic strabismus, correction of both eyes seems beneficial. The effect size of the Yokoyama procedure appears to be mainly driven by preoperative esotropia.

Published

2021

11. Biallelic mutations in l-dopachrome tautomerase (DCT) cause infantile nystagmus and oculocutaneous albinism

Author

Volk, Alexander E., Hedergott, Andrea, Preising, Markus, Rading, Sebastian, Fricke, Julia, Herkenrath, Peter, Nurnberg, Peter, Altmueller, Janine, von Ameln, Simon, Lorenz, Birgit, Neugebauer, Antje, Karsak, Meliha, Kubisch, Christian, Volk, Alexander E., Hedergott, Andrea, Preising, Markus, Rading, Sebastian, Fricke, Julia, Herkenrath, Peter, Nurnberg, Peter, Altmueller, Janine, von Ameln, Simon, Lorenz, Birgit, Neugebauer, Antje, Karsak, Meliha, and Kubisch, Christian

Abstract

Infantile nystagmus syndrome (INS) denominates early-onset, involuntary oscillatory eye movements with different etiologies. Nystagmus is also one of the symptoms in oculocutaneus albinism (OCA), a heterogeneous disease mainly caused by defects in melanin synthesis or melanosome biogenesis. Dopachrome tautomerase (DCT, also called TYRP2) together with tyrosinase (TYR) and tyrosin-related protein 1 (TYRP1) is one of the key enzymes in melanin synthesis. Although DCT ' s role in pigmentation has been proven in different species, until now only mutations in TYR and TYRP1 have been found in patients with OCA. Detailed ophthalmological and orthoptic investigations identified a consanguineous family with two individuals with isolated infantile nystagmus and one family member with subtle signs of albinism. By whole-exome sequencing and segregation analysis, we identified the missense mutation c.176G > T (p.Gly59Val) in DCT in a homozygous state in all three affected family members. We show that this mutation results in incomplete protein maturation and targeting in vitro compatible with a partial or total loss of function. Subsequent screening of a cohort of patients with OCA (n = 85) and INS (n = 25) revealed two heterozygous truncating mutations, namely c.876C > A (p.Tyr292*) and c.1407G > A (p.Trp469*), in an independent patient with OCA. Taken together, our data suggest that mutations in DCT can cause a phenotypic spectrum ranging from isolated infantile nystagmus to oculocutaneous albinism.

Published

2021

12. Screening for retinopathy of prematurity-the most important changes in the new German guidelines 2020

Author

Li, Jeany Q., Kellner, Ulrich, Lorenz, Birgit, Stahl, Andreas, Krohne, Tim U., Li, Jeany Q., Kellner, Ulrich, Lorenz, Birgit, Stahl, Andreas, and Krohne, Tim U.

Abstract

Background Due to improvements in neonatal care of premature infants and the development of novel treatment options for retinopathy of prematurity (ROP), the requirements for screening for ROP have changed since publication of the last version of the German ROP screening guideline in 2008. Based on results of recent studies, the guideline has been extensively revised in 2020 and published in an updated version. Objective This article summarizes the most important changes in the new guideline. Results The age limit for screening inclusion was lowered to a gestational age of below 31 weeks for infants without additional risk factors. The minimum duration of oxygen supplementation necessitating screening inclusion in preterm infants was increased to more than 5 days. Treatment for ROP in zone II can now be given at any stage 3 with plus disease, regardless of the number of clock hours affected. Criteria for the frequency and duration have been defined for follow-up examinations after anti-vascular endothelial growth factor (VEGF) treatment. The binding document for these and other new recommendations is the guideline itself. Conclusion The guideline recommendations enable a reliable identification of infants at risk for ROP for screening inclusion and a timely detection of advanced disease stages for treatment initiation, thus preventing blindness from ROP.

Published

2021

13. Rhabdoid Tumour of the Orbit in a Child

Author

Wilms, Vlada, Jaeger, Melanie, Schlamann, Marc, Weber, Damien Charles, Lorenz, Birgit, Wilms, Vlada, Jaeger, Melanie, Schlamann, Marc, Weber, Damien Charles, and Lorenz, Birgit

Published

2021

14. International Classification of Retinopathy of Prematurity, Third Edition

Author

Chiang, Michael F., Quinn, Graham E., Fielder, Alistair R., Ostmo, Susan R., Chan, R. V. Paul, Berrocal, Audina, Binenbaum, Gil, Blair, Michael, Campbell, J. Peter, Capone, Antonio, Chen, Yi, Dai, Shuan, Ells, Anna, Fleck, Brian W., Good, William V., Hartnett, M. Elizabeth, Holmström, Gerd, Kusaka, Shunji, Kychenthal, Andres, Lepore, Domenico, Lorenz, Birgit, Martinez-Castellanos, Maria Ana, Ozdek, Sengul, Ademola-Popoola, Dupe, Reynolds, James D., Shah, Parag K., Shapiro, Michael, Stahl, Andreas, Toth, Cynthia, Vinekar, Anand, Visser, Linda, Wallace, David K., Wu, Wei-Chi, Zhao, Peiquan, Zin, Andrea, Chiang, Michael F., Quinn, Graham E., Fielder, Alistair R., Ostmo, Susan R., Chan, R. V. Paul, Berrocal, Audina, Binenbaum, Gil, Blair, Michael, Campbell, J. Peter, Capone, Antonio, Chen, Yi, Dai, Shuan, Ells, Anna, Fleck, Brian W., Good, William V., Hartnett, M. Elizabeth, Holmström, Gerd, Kusaka, Shunji, Kychenthal, Andres, Lepore, Domenico, Lorenz, Birgit, Martinez-Castellanos, Maria Ana, Ozdek, Sengul, Ademola-Popoola, Dupe, Reynolds, James D., Shah, Parag K., Shapiro, Michael, Stahl, Andreas, Toth, Cynthia, Vinekar, Anand, Visser, Linda, Wallace, David K., Wu, Wei-Chi, Zhao, Peiquan, and Zin, Andrea

Abstract

Purpose: The International Classification of Retinopathy of Prematurity is a consensus statement that creates a standard nomenclature for classification of retinopathy of prematurity (ROP). It was initially published in 1984, expanded in 1987, and revisited in 2005. This article presents a third revision, the International Classification of Retinopathy of Prematurity, Third Edition (ICROP3), which is now required because of challenges such as: (1) concerns about subjectivity in critical elements of disease classification; (2) innovations in ophthalmic imaging; (3) novel pharmacologic therapies (e.g., antievascular endothelial growth factor agents) with unique regression and reactivation features after treatment compared with ablative therapies; and (4) recognition that patterns of ROP in some regions of the world do not fit neatly into the current classification system. Design: Review of evidence-based literature, along with expert consensus opinion. Participants: International ROP expert committee assembled in March 2019 representing 17 countries and comprising 14 pediatric ophthalmologists and 20 retinal specialists, as well as 12 women and 22 men. Methods: The committee was initially divided into 3 subcommittees-acute phase, regression or reactivation, and imaging-each of which used iterative videoconferences and an online message board to identify key challenges and approaches. Subsequently, the entire committee used iterative videoconferences, 2 in-person multiday meetings, and an online message board to develop consensus on classification. Main Outcome Measures: Consensus statement. Results: The ICROP3 retains current definitions such as zone (location of disease), stage (appearance of disease at the avascular-vascular junction), and circumferential extent of disease. Major updates in the ICROP3 include refined classification metrics (e.g., posterior zone II, notch, subcategorization of stage 5, and recognition that a continuous spectrum of vascular abnormalit

Published

2021

15. Yokoyama procedure for esotropia associated with high myopia: real-world data from a large-scale multicentre analysis

Author

Wabbels, Bettina, Fricke, Julia, Schittkowski, Michael, Graf, Michael, Lorenz, Birgit, Bau, Viktoria, Nentwich, Martin M., Atili, Abed, Eckstein, Anja, Sturm, Veit, Beisse, Christina, Sterker, Ina, Neppert, Birte, Mauschitz, Matthias M., Wabbels, Bettina, Fricke, Julia, Schittkowski, Michael, Graf, Michael, Lorenz, Birgit, Bau, Viktoria, Nentwich, Martin M., Atili, Abed, Eckstein, Anja, Sturm, Veit, Beisse, Christina, Sterker, Ina, Neppert, Birte, and Mauschitz, Matthias M.

Abstract

Purpose High myopic patients may develop strabismus due to globe dislocation out of the normal extraocular muscle cone. Surgical correction of this strabismus type is possible by joining the superior and lateral rectus muscles without the need for a scleral suture called the Yokoyama procedure. Data from large patient samples and the evaluation of a potential effect of an additional medial rectus recession (MRR) have been lacking so far. Methods We pooled retrospective patient data of 14 departments of ophthalmology in Germany and Switzerland and analysed determinants of postoperative results using multivariable regression models. Results We included 133 patients (mean age: 59.7 +/- 13.4 years, surgery between 2008 and 2017) with a mean preoperative esotropia (both Yokoyama with and without MRR) of 23.8 degrees +/- 4.6 degrees. The angle of preoperative esotropia increased with age. The postoperative esotropia was 8.7 degrees +/- 9.9 degrees, and six patients were overcorrected. While preoperative esotropia was highly associated with postoperative results, we found no association of additional MRR with any of our postoperative outcome measures. The Yokoyama procedure had a higher absolute effect in patients with higher preoperative esotropia. Conclusion Our study confirms the positive effect of the Yokoyama procedure on strabismus due to high myopia in large-scale real-world data. In some cases, MRR may be needed because of muscle contracture, although additional MRR statistically did not affect the postoperative outcome. In patients with bilateral high myopic strabismus, correction of both eyes seems beneficial. The effect size of the Yokoyama procedure appears to be mainly driven by preoperative esotropia.

Published

2021

16. Biallelic mutations in l-dopachrome tautomerase (DCT) cause infantile nystagmus and oculocutaneous albinism

Author

Volk, Alexander E., Hedergott, Andrea, Preising, Markus, Rading, Sebastian, Fricke, Julia, Herkenrath, Peter, Nurnberg, Peter, Altmueller, Janine, von Ameln, Simon, Lorenz, Birgit, Neugebauer, Antje, Karsak, Meliha, Kubisch, Christian, Volk, Alexander E., Hedergott, Andrea, Preising, Markus, Rading, Sebastian, Fricke, Julia, Herkenrath, Peter, Nurnberg, Peter, Altmueller, Janine, von Ameln, Simon, Lorenz, Birgit, Neugebauer, Antje, Karsak, Meliha, and Kubisch, Christian

Abstract

Infantile nystagmus syndrome (INS) denominates early-onset, involuntary oscillatory eye movements with different etiologies. Nystagmus is also one of the symptoms in oculocutaneus albinism (OCA), a heterogeneous disease mainly caused by defects in melanin synthesis or melanosome biogenesis. Dopachrome tautomerase (DCT, also called TYRP2) together with tyrosinase (TYR) and tyrosin-related protein 1 (TYRP1) is one of the key enzymes in melanin synthesis. Although DCT ' s role in pigmentation has been proven in different species, until now only mutations in TYR and TYRP1 have been found in patients with OCA. Detailed ophthalmological and orthoptic investigations identified a consanguineous family with two individuals with isolated infantile nystagmus and one family member with subtle signs of albinism. By whole-exome sequencing and segregation analysis, we identified the missense mutation c.176G > T (p.Gly59Val) in DCT in a homozygous state in all three affected family members. We show that this mutation results in incomplete protein maturation and targeting in vitro compatible with a partial or total loss of function. Subsequent screening of a cohort of patients with OCA (n = 85) and INS (n = 25) revealed two heterozygous truncating mutations, namely c.876C > A (p.Tyr292*) and c.1407G > A (p.Trp469*), in an independent patient with OCA. Taken together, our data suggest that mutations in DCT can cause a phenotypic spectrum ranging from isolated infantile nystagmus to oculocutaneous albinism.

Published

2021

17. Screening for retinopathy of prematurity-the most important changes in the new German guidelines 2020

Author

Li, Jeany Q., Kellner, Ulrich, Lorenz, Birgit, Stahl, Andreas, Krohne, Tim U., Li, Jeany Q., Kellner, Ulrich, Lorenz, Birgit, Stahl, Andreas, and Krohne, Tim U.

Abstract

Background Due to improvements in neonatal care of premature infants and the development of novel treatment options for retinopathy of prematurity (ROP), the requirements for screening for ROP have changed since publication of the last version of the German ROP screening guideline in 2008. Based on results of recent studies, the guideline has been extensively revised in 2020 and published in an updated version. Objective This article summarizes the most important changes in the new guideline. Results The age limit for screening inclusion was lowered to a gestational age of below 31 weeks for infants without additional risk factors. The minimum duration of oxygen supplementation necessitating screening inclusion in preterm infants was increased to more than 5 days. Treatment for ROP in zone II can now be given at any stage 3 with plus disease, regardless of the number of clock hours affected. Criteria for the frequency and duration have been defined for follow-up examinations after anti-vascular endothelial growth factor (VEGF) treatment. The binding document for these and other new recommendations is the guideline itself. Conclusion The guideline recommendations enable a reliable identification of infants at risk for ROP for screening inclusion and a timely detection of advanced disease stages for treatment initiation, thus preventing blindness from ROP.

Published

2021

18. Rhabdoid Tumour of the Orbit in a Child

Author

Wilms, Vlada, Jaeger, Melanie, Schlamann, Marc, Weber, Damien Charles, Lorenz, Birgit, Wilms, Vlada, Jaeger, Melanie, Schlamann, Marc, Weber, Damien Charles, and Lorenz, Birgit

Published

2021

19. Safety, Efficacy and Protective Aspects of an Add-on Paracentesis during Intravitreal Injections

Author

Koss, Michael Janusz, Bolz, Matthias, Augustin, Albert J., Koch, Frank, Szurman, Peter, Stanzel, Boris, Fauser, Sascha, Mennel, Stefan, Vossmerbaeumer, Urs, de Smet, Marc D., Hoehn, Fabian, Kuechle, Michael, Lorenz, Birgit, Lueke, Mathias, Lytvynchuk, Lyubomyr, Meyer, Carsten H., Paul, Christoph, Rodrigues, Eduardo B., Schrage, Norbert, Zehnder, Claus, Koss, Michael Janusz, Bolz, Matthias, Augustin, Albert J., Koch, Frank, Szurman, Peter, Stanzel, Boris, Fauser, Sascha, Mennel, Stefan, Vossmerbaeumer, Urs, de Smet, Marc D., Hoehn, Fabian, Kuechle, Michael, Lorenz, Birgit, Lueke, Mathias, Lytvynchuk, Lyubomyr, Meyer, Carsten H., Paul, Christoph, Rodrigues, Eduardo B., Schrage, Norbert, and Zehnder, Claus

Published

2020

20. Rhabdoid Tumour of the Orbit in a Child

Author

Wilms, Vlada, Jaeger, Melanie, Schlamann, Marc, Weber, Damien Charles, Lorenz, Birgit, Wilms, Vlada, Jaeger, Melanie, Schlamann, Marc, Weber, Damien Charles, and Lorenz, Birgit

Published

2020

21. Safety, Efficacy and Protective Aspects of an Add-on Paracentesis during Intravitreal Injections

Author

Koss, Michael Janusz, Bolz, Matthias, Augustin, Albert J., Koch, Frank, Szurman, Peter, Stanzel, Boris, Fauser, Sascha, Mennel, Stefan, Vossmerbaeumer, Urs, de Smet, Marc D., Hoehn, Fabian, Kuechle, Michael, Lorenz, Birgit, Lueke, Mathias, Lytvynchuk, Lyubomyr, Meyer, Carsten H., Paul, Christoph, Rodrigues, Eduardo B., Schrage, Norbert, Zehnder, Claus, Koss, Michael Janusz, Bolz, Matthias, Augustin, Albert J., Koch, Frank, Szurman, Peter, Stanzel, Boris, Fauser, Sascha, Mennel, Stefan, Vossmerbaeumer, Urs, de Smet, Marc D., Hoehn, Fabian, Kuechle, Michael, Lorenz, Birgit, Lueke, Mathias, Lytvynchuk, Lyubomyr, Meyer, Carsten H., Paul, Christoph, Rodrigues, Eduardo B., Schrage, Norbert, and Zehnder, Claus

Published

2020

22. Rhabdoid Tumour of the Orbit in a Child

Author

Wilms, Vlada, Jaeger, Melanie, Schlamann, Marc, Weber, Damien Charles, Lorenz, Birgit, Wilms, Vlada, Jaeger, Melanie, Schlamann, Marc, Weber, Damien Charles, and Lorenz, Birgit

Published

2020

23. Multirater Validation of Peripapillary Hyperreflective Ovoid Mass-like Structures (PHOMS)

Author

Petzold, Axel, Biousse, Valerie, Bursztyn, Lulu, Costello, Fiona, Crum, Alison, Digre, Kathleen, Fraser, Clare, Fraser, J. Alex, Katz, Bradley, Jurkute, Neringa, Newman, Nancy, Lautrup-Battistini, Jette, Lawlor, Mitchell, Liskova, Petra, Lorenz, Birgit, Malmqvist, Lasse, Peragallo, Jason, Sibony, Patrick, Subramanian, Prem, Rejdak, Robert, Nowomiejska, Katarzyna, Touitou, Valerie, Warner, Judith, Wegener, Marianne, Wong, Sui, Yu-Wai-Man, Patrick, Hamann, Steffen, Petzold, Axel, Biousse, Valerie, Bursztyn, Lulu, Costello, Fiona, Crum, Alison, Digre, Kathleen, Fraser, Clare, Fraser, J. Alex, Katz, Bradley, Jurkute, Neringa, Newman, Nancy, Lautrup-Battistini, Jette, Lawlor, Mitchell, Liskova, Petra, Lorenz, Birgit, Malmqvist, Lasse, Peragallo, Jason, Sibony, Patrick, Subramanian, Prem, Rejdak, Robert, Nowomiejska, Katarzyna, Touitou, Valerie, Warner, Judith, Wegener, Marianne, Wong, Sui, Yu-Wai-Man, Patrick, and Hamann, Steffen

Abstract

Peripapillary hyperreflective ovoid mass-like structures (PHOMS) are a new retinal optical coherence tomography (OCT) finding. The Optic Disc Drusen Studies Consortium had made recommendations to distinguish PHOMS from true optic disc drusen (ODD) in 2018. While publications on PHOMS have increased since then, the accuracy of the definition of PHOMS and reliability of detection is unknown. In this multi-rater study, we demonstrate that the 2018 definition of PHOMS resulted in a poor multi-rater kappa of 0.356. We performed a Delphi consensus process to develop a consistent and refined definition of PHOMS with clear principles around the nature of PHOMS and how they differ from normal anatomy. Fifty explanatory teaching slides, provided as supplementary material, allowed our expert group of raters to achieve a good level of agreement (kappa 0.701, 50 OCT scans, 21 raters). We recommend adopting the refined definition for PHOMS.

Published

2020

24. Visual impairment and blindness in institutionalized elderly in Germany

Author

Larsen, Petra P., Thiele, Sarah, Krohne, Tim U., Ziemssen, Focke, Krummenauer, Frank, Holz, Frank G., Finger, Robert P., Kohnen, Thomas, Naycheva, Lubka, Jochem, Maximilian, Reinhard, Thomas, Boehringer, Daniel, Engesser, Diana, Lagreze, Wolf, Mueller, Claudia, Wolff, Carolin, Schmitz, Jessica, Lorenz, Birgit, Papadopoulou-Laiou, Chrysanthi, Holve, Kerstin, Schweinfurth, Silke, Hoerauf, Hans, Schwarz, Wiebke, Spitzer, Martin, Wagenfeld, Lars, Bertram, Paul, Auffarth, Gerd, Gavrilovic, Branka, Cursiefen, Claus, Schaub, Friederike, Lentzsch, Anna, Welsandt, Gerhard, Thieme, Hagen, Weigel, Melanie, Hidaya, Diyala, Ehmer, Angela, Priglinger, Siegfried, von Livonius, Bettina, Drexler, Carina, Semmelsberger, Jessica, Eter, Nicole, Alten, Florian, Sigleur, Annika, Sieber, Dorothee, Braeutigam, Andrea, Haerter, Friederike, Adorf, Adeline, Pauleikhoff, Daniel, Robering, Angela, Helbig, Horst, Brandl, Caroline, Roeck, Daniel, Tulka, Sabrina, Wabbels, Bettina, Kupitz, David. G., Goebel, Arno P., Steinberg, Julia, Schnetzer, Anne, Kobialka, Bianka, Prinz, Beate, Kutten, Danielle, Schneider, Pia, Toczko, Olivia, Yoganathan, Thanushiya, Larsen, Petra P., Thiele, Sarah, Krohne, Tim U., Ziemssen, Focke, Krummenauer, Frank, Holz, Frank G., Finger, Robert P., Kohnen, Thomas, Naycheva, Lubka, Jochem, Maximilian, Reinhard, Thomas, Boehringer, Daniel, Engesser, Diana, Lagreze, Wolf, Mueller, Claudia, Wolff, Carolin, Schmitz, Jessica, Lorenz, Birgit, Papadopoulou-Laiou, Chrysanthi, Holve, Kerstin, Schweinfurth, Silke, Hoerauf, Hans, Schwarz, Wiebke, Spitzer, Martin, Wagenfeld, Lars, Bertram, Paul, Auffarth, Gerd, Gavrilovic, Branka, Cursiefen, Claus, Schaub, Friederike, Lentzsch, Anna, Welsandt, Gerhard, Thieme, Hagen, Weigel, Melanie, Hidaya, Diyala, Ehmer, Angela, Priglinger, Siegfried, von Livonius, Bettina, Drexler, Carina, Semmelsberger, Jessica, Eter, Nicole, Alten, Florian, Sigleur, Annika, Sieber, Dorothee, Braeutigam, Andrea, Haerter, Friederike, Adorf, Adeline, Pauleikhoff, Daniel, Robering, Angela, Helbig, Horst, Brandl, Caroline, Roeck, Daniel, Tulka, Sabrina, Wabbels, Bettina, Kupitz, David. G., Goebel, Arno P., Steinberg, Julia, Schnetzer, Anne, Kobialka, Bianka, Prinz, Beate, Kutten, Danielle, Schneider, Pia, Toczko, Olivia, and Yoganathan, Thanushiya

Abstract

PurposeTo determine the prevalence of and identify factors associated with visual impairment and blindness in institutionalized elderly in Germany.MethodsIn this prospective multicenter cross-sectional study, ophthalmic health care need and provision were investigated in institutionalized elderly in 32 nursing homes in Germany. All participants underwent a standardized examination including medical and ocular history, refraction, visual acuity testing, tonometry, biomicroscopy, and dilated funduscopy. A standardized questionnaire was used to identify factors associated with eye healthcare utilization, visual impairment and/or blindness.ResultsVisual acuity of 566 (94.3%; 413 women and 153 men) of a total of 600 institutionalized elderly was determined. Mean age of the included patients was 82.9years (9.8). Of all participants, 30 (5.3%; 95% CI 3.4-7.2%) were blind and 106 (18.7%; 95% CI 15.5-21.9%) were moderately or severely visually impaired according to the World Health Organization definition. The 136 blind and moderately or severely visually impaired participants were older (OR, Odds Ratio=1.1, 95% CI 1.0-1.1; p<0.001), and more likely to have reduced mobility (OR=12.6, 95% CI 2.8-57.6; p=0.001).Conclusion p id=Par4 A high proportion of blindness and visual impairment was found amongst nursing home residents. Age and reduced mobility were factors associated with an increased likelihood of blindness and visual impairment. Any surveys of blindness and visual impairment excluding nursing homes may considerably underestimate the prevalence of visual impairment and blindness.

Published

2019

25. Biallelic mutation of human SLC6A6 encoding the taurine transporter TAUT is linked to early retinal degeneration

Author

Preising, Markus N., Goerg, Boris, Friedburg, Christoph, Qvartskhava, Natalia, Budde, Birgit S., Bonus, Michele, Toliat, Mohammad R., Pfleger, Christopher, Altmueller, Janine, Herebian, Diran, Beyer, Mila, Zoellner, Helge J., Wittsack, Hans-Joerg, Schaper, Joerg, Klee, Dirk, Zechner, Ulrich, Nuernberg, Peter, Schipper, Joerg, Schnitzler, Alfons, Gohlke, Holger, Lorenz, Birgit, Haeussinger, Dieter, Bolz, Hanno J., Preising, Markus N., Goerg, Boris, Friedburg, Christoph, Qvartskhava, Natalia, Budde, Birgit S., Bonus, Michele, Toliat, Mohammad R., Pfleger, Christopher, Altmueller, Janine, Herebian, Diran, Beyer, Mila, Zoellner, Helge J., Wittsack, Hans-Joerg, Schaper, Joerg, Klee, Dirk, Zechner, Ulrich, Nuernberg, Peter, Schipper, Joerg, Schnitzler, Alfons, Gohlke, Holger, Lorenz, Birgit, Haeussinger, Dieter, and Bolz, Hanno J.

Abstract

We previously reported that inactivation of the transmembrane taurine transporter (TauT or solute carrier 6a6) causes early retinal degeneration in mice. Compatible with taurine's indispensability for cell volume homeostasis, protein stabilization, cytoprotection, antioxidation, and immuno- and neuromodulation, mice develop multisystemic dysfunctions (hearing loss; liver fibrosis; and behavioral, heart, and skeletal muscle abnormalities) later on. Here, by genetic, cell biologic, in vivo H-1-magnetic resonance spectroscopy and molecular dynamics simulation studies, we conducted in-depth characterization of a novel disorder: human TAUT deficiency. Loss of TAUT function due to a homozygous missense mutation caused panretinal degeneration in 2 brothers. TAUT(p.A78E) still localized in the plasma membrane but is predicted to impact structural stabilization. H-3-taurine uptake by peripheral blood mononuclear cells was reduced by 95%, and taurine levels were severely reduced in plasma, skeletal muscle, and brain. Extraocular dysfunctions were not yet detected, but significantly increased urinary excretion of 8-oxo-7,8-dihydroguanosine indicated generally enhanced (yet clinically unapparent) oxidative stress and RNA oxidation, warranting continuous broad surveillance.-Preising, M. N., Gorg, B., Friedburg, C., Qvartskhava, N., Budde, B. S., Bonus, M., Toliat, M. R., Pfleger, C., Altmuller, J., Herebian, D., Beyer, M., Zollner, H. J., Wittsack, H.-J., Schaper, J., Klee, D., Zechner, U., Nurnberg, P., Schipper, J., Schnitzler, A., Gohlke, H., Lorenz, B., Haussinger, D., Bolz, H. J. Biallelic mutation of human SLC6A6 encoding the taurine transporter TAUT is linked to early retinal degeneration.

Published

2019

26. Visual impairment and blindness in institutionalized elderly in Germany

Author

Larsen, Petra P., Thiele, Sarah, Krohne, Tim U., Ziemssen, Focke, Krummenauer, Frank, Holz, Frank G., Finger, Robert P., Kohnen, Thomas, Naycheva, Lubka, Jochem, Maximilian, Reinhard, Thomas, Boehringer, Daniel, Engesser, Diana, Lagreze, Wolf, Mueller, Claudia, Wolff, Carolin, Schmitz, Jessica, Lorenz, Birgit, Papadopoulou-Laiou, Chrysanthi, Holve, Kerstin, Schweinfurth, Silke, Hoerauf, Hans, Schwarz, Wiebke, Spitzer, Martin, Wagenfeld, Lars, Bertram, Paul, Auffarth, Gerd, Gavrilovic, Branka, Cursiefen, Claus, Schaub, Friederike, Lentzsch, Anna, Welsandt, Gerhard, Thieme, Hagen, Weigel, Melanie, Hidaya, Diyala, Ehmer, Angela, Priglinger, Siegfried, von Livonius, Bettina, Drexler, Carina, Semmelsberger, Jessica, Eter, Nicole, Alten, Florian, Sigleur, Annika, Sieber, Dorothee, Braeutigam, Andrea, Haerter, Friederike, Adorf, Adeline, Pauleikhoff, Daniel, Robering, Angela, Helbig, Horst, Brandl, Caroline, Roeck, Daniel, Tulka, Sabrina, Wabbels, Bettina, Kupitz, David. G., Goebel, Arno P., Steinberg, Julia, Schnetzer, Anne, Kobialka, Bianka, Prinz, Beate, Kutten, Danielle, Schneider, Pia, Toczko, Olivia, Yoganathan, Thanushiya, Larsen, Petra P., Thiele, Sarah, Krohne, Tim U., Ziemssen, Focke, Krummenauer, Frank, Holz, Frank G., Finger, Robert P., Kohnen, Thomas, Naycheva, Lubka, Jochem, Maximilian, Reinhard, Thomas, Boehringer, Daniel, Engesser, Diana, Lagreze, Wolf, Mueller, Claudia, Wolff, Carolin, Schmitz, Jessica, Lorenz, Birgit, Papadopoulou-Laiou, Chrysanthi, Holve, Kerstin, Schweinfurth, Silke, Hoerauf, Hans, Schwarz, Wiebke, Spitzer, Martin, Wagenfeld, Lars, Bertram, Paul, Auffarth, Gerd, Gavrilovic, Branka, Cursiefen, Claus, Schaub, Friederike, Lentzsch, Anna, Welsandt, Gerhard, Thieme, Hagen, Weigel, Melanie, Hidaya, Diyala, Ehmer, Angela, Priglinger, Siegfried, von Livonius, Bettina, Drexler, Carina, Semmelsberger, Jessica, Eter, Nicole, Alten, Florian, Sigleur, Annika, Sieber, Dorothee, Braeutigam, Andrea, Haerter, Friederike, Adorf, Adeline, Pauleikhoff, Daniel, Robering, Angela, Helbig, Horst, Brandl, Caroline, Roeck, Daniel, Tulka, Sabrina, Wabbels, Bettina, Kupitz, David. G., Goebel, Arno P., Steinberg, Julia, Schnetzer, Anne, Kobialka, Bianka, Prinz, Beate, Kutten, Danielle, Schneider, Pia, Toczko, Olivia, and Yoganathan, Thanushiya

Abstract

PurposeTo determine the prevalence of and identify factors associated with visual impairment and blindness in institutionalized elderly in Germany.MethodsIn this prospective multicenter cross-sectional study, ophthalmic health care need and provision were investigated in institutionalized elderly in 32 nursing homes in Germany. All participants underwent a standardized examination including medical and ocular history, refraction, visual acuity testing, tonometry, biomicroscopy, and dilated funduscopy. A standardized questionnaire was used to identify factors associated with eye healthcare utilization, visual impairment and/or blindness.ResultsVisual acuity of 566 (94.3%; 413 women and 153 men) of a total of 600 institutionalized elderly was determined. Mean age of the included patients was 82.9years (9.8). Of all participants, 30 (5.3%; 95% CI 3.4-7.2%) were blind and 106 (18.7%; 95% CI 15.5-21.9%) were moderately or severely visually impaired according to the World Health Organization definition. The 136 blind and moderately or severely visually impaired participants were older (OR, Odds Ratio=1.1, 95% CI 1.0-1.1; p<0.001), and more likely to have reduced mobility (OR=12.6, 95% CI 2.8-57.6; p=0.001).Conclusion p id=Par4 A high proportion of blindness and visual impairment was found amongst nursing home residents. Age and reduced mobility were factors associated with an increased likelihood of blindness and visual impairment. Any surveys of blindness and visual impairment excluding nursing homes may considerably underestimate the prevalence of visual impairment and blindness.

Published

2019

27. Biallelic mutation of human SLC6A6 encoding the taurine transporter TAUT is linked to early retinal degeneration

Author

Preising, Markus N., Goerg, Boris, Friedburg, Christoph, Qvartskhava, Natalia, Budde, Birgit S., Bonus, Michele, Toliat, Mohammad R., Pfleger, Christopher, Altmueller, Janine, Herebian, Diran, Beyer, Mila, Zoellner, Helge J., Wittsack, Hans-Joerg, Schaper, Joerg, Klee, Dirk, Zechner, Ulrich, Nuernberg, Peter, Schipper, Joerg, Schnitzler, Alfons, Gohlke, Holger, Lorenz, Birgit, Haeussinger, Dieter, Bolz, Hanno J., Preising, Markus N., Goerg, Boris, Friedburg, Christoph, Qvartskhava, Natalia, Budde, Birgit S., Bonus, Michele, Toliat, Mohammad R., Pfleger, Christopher, Altmueller, Janine, Herebian, Diran, Beyer, Mila, Zoellner, Helge J., Wittsack, Hans-Joerg, Schaper, Joerg, Klee, Dirk, Zechner, Ulrich, Nuernberg, Peter, Schipper, Joerg, Schnitzler, Alfons, Gohlke, Holger, Lorenz, Birgit, Haeussinger, Dieter, and Bolz, Hanno J.

Abstract

We previously reported that inactivation of the transmembrane taurine transporter (TauT or solute carrier 6a6) causes early retinal degeneration in mice. Compatible with taurine's indispensability for cell volume homeostasis, protein stabilization, cytoprotection, antioxidation, and immuno- and neuromodulation, mice develop multisystemic dysfunctions (hearing loss; liver fibrosis; and behavioral, heart, and skeletal muscle abnormalities) later on. Here, by genetic, cell biologic, in vivo H-1-magnetic resonance spectroscopy and molecular dynamics simulation studies, we conducted in-depth characterization of a novel disorder: human TAUT deficiency. Loss of TAUT function due to a homozygous missense mutation caused panretinal degeneration in 2 brothers. TAUT(p.A78E) still localized in the plasma membrane but is predicted to impact structural stabilization. H-3-taurine uptake by peripheral blood mononuclear cells was reduced by 95%, and taurine levels were severely reduced in plasma, skeletal muscle, and brain. Extraocular dysfunctions were not yet detected, but significantly increased urinary excretion of 8-oxo-7,8-dihydroguanosine indicated generally enhanced (yet clinically unapparent) oxidative stress and RNA oxidation, warranting continuous broad surveillance.-Preising, M. N., Gorg, B., Friedburg, C., Qvartskhava, N., Budde, B. S., Bonus, M., Toliat, M. R., Pfleger, C., Altmuller, J., Herebian, D., Beyer, M., Zollner, H. J., Wittsack, H.-J., Schaper, J., Klee, D., Zechner, U., Nurnberg, P., Schipper, J., Schnitzler, A., Gohlke, H., Lorenz, B., Haussinger, D., Bolz, H. J. Biallelic mutation of human SLC6A6 encoding the taurine transporter TAUT is linked to early retinal degeneration.

Published

2019

28. The Natural History of Inherited Retinal Dystrophy Due to Biallelic Mutations in the RPE65 Gene

Author

Chung, Daniel C, Bertelsen, Mette, Lorenz, Birgit, Pennesi, Mark E, Leroy, Bart P, Hamel, Christian P, Pierce, Eric, Sallum, Juliana, Larsen, Michael, Stieger, Knut, Preising, Markus, Weleber, Richard, Yang, Paul, Place, Emily, Liu, Emily, Schaefer, Grace, DiStefano-Pappas, Julie, Elci, Okan U, McCague, Sarah, Wellman, Jennifer A, High, Katherine A, Reape, Kathleen Z, Chung, Daniel C, Bertelsen, Mette, Lorenz, Birgit, Pennesi, Mark E, Leroy, Bart P, Hamel, Christian P, Pierce, Eric, Sallum, Juliana, Larsen, Michael, Stieger, Knut, Preising, Markus, Weleber, Richard, Yang, Paul, Place, Emily, Liu, Emily, Schaefer, Grace, DiStefano-Pappas, Julie, Elci, Okan U, McCague, Sarah, Wellman, Jennifer A, High, Katherine A, and Reape, Kathleen Z

Abstract

PURPOSE: To delineate the natural history of visual parameters over time in individuals with biallelic RPE65 mutation-associated inherited retinal dystrophy (IRD); describe the range of causative mutations; determine potential genotype/phenotype relationships; and describe the variety of clinical diagnoses.DESIGN: Global, multicenter, retrospective chart review.METHODS: Study Population: Seventy individuals with biallelic RPE65 mutation-associated IRD.PROCEDURES: Data were extracted from patient charts.MEASUREMENTS: Visual acuity (VA), Goldmann visual field (GVF), optical coherence tomography, color vision testing, light sensitivity testing, and electroretinograms (retinal imaging and fundus photography were collected and analyzed when available).RESULTS: VA decreased with age in a nonlinear, positive-acceleration relationship (P < .001). GVF decreased with age (P < .0001 for both V4e and III4e), with faster GVF decrease for III4e stimulus vs V4e (P = .0114, left eye; P = .0076, right eye). On average, a 1-year increase in age decreased III4e GVF by ∼25 sum total degrees in each eye while V4e GVF decreased by ∼37 sum total degrees in each eye, although individual variability was observed. A total of 78 clinical diagnoses and 56 unique RPE65 mutations were recorded, without discernible RPE65 mutation genotype/phenotype relationships.CONCLUSIONS: The number of clinical diagnoses and lack of a consistent RPE65 mutation-to-phenotype correlation underscore the need for genetic testing. Significant relationships between age and worsening VA and GVF highlight the progressive loss of functional retina over time. These data may have implications for optimal timing of treatment for IRD attributable to biallelic RPE65 mutations.

Published

2019

29. Recurrent heterozygous PAX6 missense variants cause severe bilateral microphthalmia via predictable effects on DNA–protein interaction

Author

Williamson, Kathleen K.A., Hall, Hildegard Nikki, Owen, Liusaidh L.J., Livesey, Benjamin B.J., Hanson, Isabel I.M., Adams, Gillian Gwendolen G.G.W., Bodek, Simon, Calvas, Patrick, Castle, Bruce, Clarke, Michael, Deng, Alexander A.T., Edery, Patrick, Fisher, Richard R.S., Gillessen-Kaesbach, Gabriele, Heon, Elise, Hurst, Jane, Josifova, Dragana, Lorenz, Birgit, McKee, Shane, Meire, Françoise, Moore, Anthony Thomas, Parker, Michael W, Reiff, Charlotte C.M., Self, Jay, Tobias, Edward E.S., Verheij, Joke BGM G M J., Willems, Marjolaine, Williams, Denise, Van Heyningen, Veronica, Marsh, Joseph Arthur, FitzPatrick, David D.R., Williamson, Kathleen K.A., Hall, Hildegard Nikki, Owen, Liusaidh L.J., Livesey, Benjamin B.J., Hanson, Isabel I.M., Adams, Gillian Gwendolen G.G.W., Bodek, Simon, Calvas, Patrick, Castle, Bruce, Clarke, Michael, Deng, Alexander A.T., Edery, Patrick, Fisher, Richard R.S., Gillessen-Kaesbach, Gabriele, Heon, Elise, Hurst, Jane, Josifova, Dragana, Lorenz, Birgit, McKee, Shane, Meire, Françoise, Moore, Anthony Thomas, Parker, Michael W, Reiff, Charlotte C.M., Self, Jay, Tobias, Edward E.S., Verheij, Joke BGM G M J., Willems, Marjolaine, Williams, Denise, Van Heyningen, Veronica, Marsh, Joseph Arthur, and FitzPatrick, David D.R.

Abstract

Purpose: Most classical aniridia is caused by PAX6 haploinsufficiency. PAX6 missense variants can be hypomorphic or mimic haploinsufficiency. We hypothesized that missense variants also cause previously undescribed disease by altering the affinity and/or specificity of PAX6 genomic interactions. Methods: We screened PAX6 in 372 individuals with bilateral microphthalmia, anophthalmia, or coloboma (MAC) from the Medical Research Council Human Genetics Unit eye malformation cohort (HGUeye) and reviewed data from the Deciphering Developmental Disorders study. We performed cluster analysis on PAX6-associated ocular phenotypes by variant type and molecular modeling of the structural impact of 86 different PAX6 causative missense variants. Results: Eight different PAX6 missense variants were identified in 17 individuals (15 families) with MAC, accounting for 4% (15/372) of our cohort. Seven altered the paired domain (p.[Arg26Gln]x1, p.[Gly36Val]x1, p.[Arg38Trp]x2, p.[Arg38Gln]x1, p.[Gly51Arg]x2, p.[Ser54Arg]x2, p.[Asn124Lys]x5) and one the homeodomain (p.[Asn260Tyr]x1). p.Ser54Arg and p.Asn124Lys were exclusively associated with severe bilateral microphthalmia. MAC-associated variants were predicted to alter but not ablate DNA interaction, consistent with the electrophoretic mobility shifts observed using mutant paired domains with well-characterized PAX6-binding sites. We found no strong evidence for novel PAX6-associated extraocular disease. Conclusion: Altering the affinity and specificity of PAX6-binding genome-wide provides a plausible mechanism for the worse-than-null effects of MAC-associated missense variants., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2019

30. Clinical Characterization of 66 Patients With Congenital Retinal Disease Due to the Deep-Intronic c.2991+11655A > G Mutation in CEP290

Author

Valkenburg, D., Cauwenbergh, Caroline Van, Lorenz, Birgit, Genderen, M.M. van, Bertelsen, Mette, Pott, J.W., Klaver, C.C.W., Hoyng, C.B., Born, L.I. van den, Collin, R.W.J., Valkenburg, D., Cauwenbergh, Caroline Van, Lorenz, Birgit, Genderen, M.M. van, Bertelsen, Mette, Pott, J.W., Klaver, C.C.W., Hoyng, C.B., Born, L.I. van den, and Collin, R.W.J.

Abstract

Contains fulltext : 195435.pdf (Publisher’s version ) (Open Access)

Published

2018

31. Clinical characterization of 66 patients with congenital retinal disease due to the deep-intronic c.2991+1655A>G mutation in CEP290

Author

Valkenburg, Dyon, van Cauwenbergh, Caroline, Lorenz, Birgit, van Genderen, Mies M., Bertelsen, Mette, Pott, Jan Willem R., Coppieters, Frauke, de Zaeytijd, Julie, Thiadens, Alberta A.H.J., Klaver, Caroline C.W., Kroes, Hester Y., van Schooneveld, Mary J., Preising, Markus, Hoyng, Carel B., Leroy, Bart P., Ingeborgh van den Born, L., Collin, Rob W.J., Valkenburg, Dyon, van Cauwenbergh, Caroline, Lorenz, Birgit, van Genderen, Mies M., Bertelsen, Mette, Pott, Jan Willem R., Coppieters, Frauke, de Zaeytijd, Julie, Thiadens, Alberta A.H.J., Klaver, Caroline C.W., Kroes, Hester Y., van Schooneveld, Mary J., Preising, Markus, Hoyng, Carel B., Leroy, Bart P., Ingeborgh van den Born, L., and Collin, Rob W.J.

Published

2018

32. Clinical characterization of 66 patients with congenital retinal disease due to the deep-intronic c.2991+1655A>G mutation in CEP290

Author

Valkenburg, Dyon, van Cauwenbergh, Caroline, Lorenz, Birgit, van Genderen, Mies M., Bertelsen, Mette, Pott, Jan Willem R., Coppieters, Frauke, de Zaeytijd, Julie, Thiadens, Alberta A.H.J., Klaver, Caroline C.W., Kroes, Hester Y., van Schooneveld, Mary J., Preising, Markus, Hoyng, Carel B., Leroy, Bart P., Ingeborgh van den Born, L., Collin, Rob W.J., Valkenburg, Dyon, van Cauwenbergh, Caroline, Lorenz, Birgit, van Genderen, Mies M., Bertelsen, Mette, Pott, Jan Willem R., Coppieters, Frauke, de Zaeytijd, Julie, Thiadens, Alberta A.H.J., Klaver, Caroline C.W., Kroes, Hester Y., van Schooneveld, Mary J., Preising, Markus, Hoyng, Carel B., Leroy, Bart P., Ingeborgh van den Born, L., and Collin, Rob W.J.

Published

2018

33. Clinical Characterization of 66 Patients With Congenital Retinal Disease Due to the Deep-Intronic c.2991+11655A > G Mutation in CEP290

Author

Valkenburg, D., Cauwenbergh, Caroline Van, Lorenz, Birgit, Genderen, M.M. van, Bertelsen, Mette, Pott, J.W., Klaver, C.C.W., Hoyng, C.B., Born, L.I. van den, Collin, R.W.J., Valkenburg, D., Cauwenbergh, Caroline Van, Lorenz, Birgit, Genderen, M.M. van, Bertelsen, Mette, Pott, J.W., Klaver, C.C.W., Hoyng, C.B., Born, L.I. van den, and Collin, R.W.J.

Abstract

Contains fulltext : 195435.pdf (Publisher’s version ) (Open Access)

Published

2018

34. Clinical characterization of 66 patients with congenital retinal disease due to the deep-intronic c.2991+1655A>G mutation in CEP290

Author

Valkenburg, Dyon, van Cauwenbergh, Caroline, Lorenz, Birgit, van Genderen, Mies M., Bertelsen, Mette, Pott, Jan Willem R., Coppieters, Frauke, de Zaeytijd, Julie, Thiadens, Alberta A.H.J., Klaver, Caroline C.W., Kroes, Hester Y., van Schooneveld, Mary J., Preising, Markus, Hoyng, Carel B., Leroy, Bart P., Ingeborgh van den Born, L., Collin, Rob W.J., Valkenburg, Dyon, van Cauwenbergh, Caroline, Lorenz, Birgit, van Genderen, Mies M., Bertelsen, Mette, Pott, Jan Willem R., Coppieters, Frauke, de Zaeytijd, Julie, Thiadens, Alberta A.H.J., Klaver, Caroline C.W., Kroes, Hester Y., van Schooneveld, Mary J., Preising, Markus, Hoyng, Carel B., Leroy, Bart P., Ingeborgh van den Born, L., and Collin, Rob W.J.

Published

2018

35. Clinical Characterization of 66 Patients With Congenital Retinal Disease Due to the Deep-Intronic c.2991+11655A > G Mutation in CEP290

Author

Valkenburg, D., Cauwenbergh, Caroline Van, Lorenz, Birgit, Genderen, M.M. van, Bertelsen, Mette, Pott, J.W., Klaver, C.C.W., Hoyng, C.B., Born, L.I. van den, Collin, R.W.J., Valkenburg, D., Cauwenbergh, Caroline Van, Lorenz, Birgit, Genderen, M.M. van, Bertelsen, Mette, Pott, J.W., Klaver, C.C.W., Hoyng, C.B., Born, L.I. van den, and Collin, R.W.J.

Abstract

Contains fulltext : 195435.pdf (Publisher’s version ) (Open Access)

Published

2018

36. Clinical characterization of 66 patients with congenital retinal disease due to the deep-intronic c.2991+1655A>G mutation in CEP290

Author

Genetica, Genetica Klinische Genetica, Child Health, Valkenburg, Dyon, van Cauwenbergh, Caroline, Lorenz, Birgit, van Genderen, Mies M., Bertelsen, Mette, Pott, Jan Willem R., Coppieters, Frauke, de Zaeytijd, Julie, Thiadens, Alberta A.H.J., Klaver, Caroline C.W., Kroes, Hester Y., van Schooneveld, Mary J., Preising, Markus, Hoyng, Carel B., Leroy, Bart P., Ingeborgh van den Born, L., Collin, Rob W.J., Genetica, Genetica Klinische Genetica, Child Health, Valkenburg, Dyon, van Cauwenbergh, Caroline, Lorenz, Birgit, van Genderen, Mies M., Bertelsen, Mette, Pott, Jan Willem R., Coppieters, Frauke, de Zaeytijd, Julie, Thiadens, Alberta A.H.J., Klaver, Caroline C.W., Kroes, Hester Y., van Schooneveld, Mary J., Preising, Markus, Hoyng, Carel B., Leroy, Bart P., Ingeborgh van den Born, L., and Collin, Rob W.J.

Published

2018

37. Next-generation sequencing reveals the mutational landscape of clinically diagnosed Usher syndrome: copy number variations, phenocopies, a predominant target for translational read-through, and PEX26 mutated in Heimler syndrome

Author

Neuhaus, Christine, Eisenberger, Tobias, Decker, Christian, Nagl, Sandra, Blank, Cornelia, Pfister, Markus, Kennerknecht, Ingo, Mueller-Hofstede, Cornelie, Issa, Peter Charbel, Heller, Raoul, Beck, Bodo, Ruether, Klaus, Mitter, Diana, Rohrschneider, Klaus, Steinhauer, Ute, Korbmacher, Heike M., Huhle, Dagmar, Elsayed, Solaf M., Taha, Hesham M., Baig, Shahid M., Stoehr, Heidi, Preising, Markus, Markus, Susanne, Moeller, Fabian, Lorenz, Birgit, Nagel-Wolfrum, Kerstin, Khan, Arif O., Bolz, Hanno J., Neuhaus, Christine, Eisenberger, Tobias, Decker, Christian, Nagl, Sandra, Blank, Cornelia, Pfister, Markus, Kennerknecht, Ingo, Mueller-Hofstede, Cornelie, Issa, Peter Charbel, Heller, Raoul, Beck, Bodo, Ruether, Klaus, Mitter, Diana, Rohrschneider, Klaus, Steinhauer, Ute, Korbmacher, Heike M., Huhle, Dagmar, Elsayed, Solaf M., Taha, Hesham M., Baig, Shahid M., Stoehr, Heidi, Preising, Markus, Markus, Susanne, Moeller, Fabian, Lorenz, Birgit, Nagel-Wolfrum, Kerstin, Khan, Arif O., and Bolz, Hanno J.

Abstract

BackgroundCombined retinal degeneration and sensorineural hearing impairment is mostly due to autosomal recessive Usher syndrome (USH1: congenital deafness, early retinitis pigmentosa (RP); USH2: progressive hearing impairment, RP). MethodsSanger sequencing and NGS of 112 genes (Usher syndrome, nonsyndromic deafness, overlapping conditions), MLPA, and array-CGH were conducted in 138 patients clinically diagnosed with Usher syndrome. ResultsA molecular diagnosis was achieved in 97% of both USH1 and USH2 patients, with biallelic mutations in 97% (USH1) and 90% (USH2), respectively. Quantitative readout reliably detected CNVs (confirmed by MLPA or array-CGH), qualifying targeted NGS as one tool for detecting point mutations and CNVs. CNVs accounted for 10% of identified USH2A alleles, often in trans to seemingly monoallelic point mutations. We demonstrate PTC124-induced read-through of the common p.Trp3955* nonsense mutation (13% of detected USH2A alleles), a potential therapy target. Usher gene mutations were found in most patients with atypical Usher syndrome, but the diagnosis was adjusted in case of double homozygosity for mutations in OTOA and NR2E3, genes implicated in isolated deafness and RP. Two patients with additional enamel dysplasia had biallelic PEX26 mutations, for the first time linking this gene to Heimler syndrome. ConclusionTargeted NGS not restricted to Usher genes proved beneficial in uncovering conditions mimicking Usher syndrome.

Published

2017

38. Next-generation sequencing reveals the mutational landscape of clinically diagnosed Usher syndrome: copy number variations, phenocopies, a predominant target for translational read-through, and PEX26 mutated in Heimler syndrome

Author

Neuhaus, Christine, Eisenberger, Tobias, Decker, Christian, Nagl, Sandra, Blank, Cornelia, Pfister, Markus, Kennerknecht, Ingo, Mueller-Hofstede, Cornelie, Issa, Peter Charbel, Heller, Raoul, Beck, Bodo, Ruether, Klaus, Mitter, Diana, Rohrschneider, Klaus, Steinhauer, Ute, Korbmacher, Heike M., Huhle, Dagmar, Elsayed, Solaf M., Taha, Hesham M., Baig, Shahid M., Stoehr, Heidi, Preising, Markus, Markus, Susanne, Moeller, Fabian, Lorenz, Birgit, Nagel-Wolfrum, Kerstin, Khan, Arif O., Bolz, Hanno J., Neuhaus, Christine, Eisenberger, Tobias, Decker, Christian, Nagl, Sandra, Blank, Cornelia, Pfister, Markus, Kennerknecht, Ingo, Mueller-Hofstede, Cornelie, Issa, Peter Charbel, Heller, Raoul, Beck, Bodo, Ruether, Klaus, Mitter, Diana, Rohrschneider, Klaus, Steinhauer, Ute, Korbmacher, Heike M., Huhle, Dagmar, Elsayed, Solaf M., Taha, Hesham M., Baig, Shahid M., Stoehr, Heidi, Preising, Markus, Markus, Susanne, Moeller, Fabian, Lorenz, Birgit, Nagel-Wolfrum, Kerstin, Khan, Arif O., and Bolz, Hanno J.

Abstract

BackgroundCombined retinal degeneration and sensorineural hearing impairment is mostly due to autosomal recessive Usher syndrome (USH1: congenital deafness, early retinitis pigmentosa (RP); USH2: progressive hearing impairment, RP). MethodsSanger sequencing and NGS of 112 genes (Usher syndrome, nonsyndromic deafness, overlapping conditions), MLPA, and array-CGH were conducted in 138 patients clinically diagnosed with Usher syndrome. ResultsA molecular diagnosis was achieved in 97% of both USH1 and USH2 patients, with biallelic mutations in 97% (USH1) and 90% (USH2), respectively. Quantitative readout reliably detected CNVs (confirmed by MLPA or array-CGH), qualifying targeted NGS as one tool for detecting point mutations and CNVs. CNVs accounted for 10% of identified USH2A alleles, often in trans to seemingly monoallelic point mutations. We demonstrate PTC124-induced read-through of the common p.Trp3955* nonsense mutation (13% of detected USH2A alleles), a potential therapy target. Usher gene mutations were found in most patients with atypical Usher syndrome, but the diagnosis was adjusted in case of double homozygosity for mutations in OTOA and NR2E3, genes implicated in isolated deafness and RP. Two patients with additional enamel dysplasia had biallelic PEX26 mutations, for the first time linking this gene to Heimler syndrome. ConclusionTargeted NGS not restricted to Usher genes proved beneficial in uncovering conditions mimicking Usher syndrome.

Published

2017

39. Outer plexiform layer structures are not altered following AAV-mediated gene transfer in healthy rat retina

Author

Michalakis, Stylianos, Ivanova, Elena, Palf, Arpad, Giers, Bert Constantin, Klein, Daniela, Mendes-Madeira, Alexandra, Isiegas, Carolina, Lorenz, Birgit, Haverkamp, Silke, Stieger, Knut, Michalakis, Stylianos, Ivanova, Elena, Palf, Arpad, Giers, Bert Constantin, Klein, Daniela, Mendes-Madeira, Alexandra, Isiegas, Carolina, Lorenz, Birgit, Haverkamp, Silke, and Stieger, Knut

Abstract

Ocular gene therapy approaches have been developed for a variety of different diseases. In particular, clinical gene therapy trials for RPE65 mutations, X-linked retinoschisis, and choroideremia have been conducted at different centers in recent years, showing that adeno-associated virus (AAV)-mediated gene therapy is safe, but limitations exist as to the therapeutic benefit and long-term duration of the treatment. The technique of vector delivery to retinal cells relies on subretinal injection of the vector solution, causing a transient retinal detachment. Although retinal detachments are known to cause remodeling of retinal neuronal structures as well as significant cell loss, the possible effects of this short-term therapeutic retinal detachment on retinal structure and circuitry have not yet been studied in detail. In this study, retinal morphology and apoptotic status were examined in healthy rat retinas following AAV-mediated gene transfer via subretinal injection with AAV2/5.CMV.d2GFP or sham injection with fluorescein. Outer plexiform layer (OPL) morphology was assessed by immunohistochemical labeling, laser scanning confocal microscopy, and electron microscopy. The number of synaptic contacts in the OPL was quantified after labeling with structural markers. To assess the apoptotic status, inflammatory and pro-apoptotic markers were tested and TUNEL assay for the detection of apoptotic nuclei was performed. Pre- and postsynaptic structures in the OPL, such as synaptic ribbons or horizontal and bipolar cell processes, did not differ in size or shape in injected versus non-injected areas and control retinas. Absolute numbers of synaptic ribbons were not altered. No signs of relevant gliosis were detected. TUNEL labeling of retinal cells did not vary between injected and non-injected areas, and apoptosis-inducing factor was not delocalized to the nucleus in transduced areas. The neuronal circuits in the OPL of healthy rat retinas undergoing AAV-mediated gene tr

Published

2017

40. Rebound macular edema following oral acetazolamide therapy for juvenile X-linked retinoschisis in an Italian family

Author

Galantuomo,Maria Silvana, Fossarello,Maurizio, Cuccu,Alberto, Farci,Roberta, Preising,Markus N, Lorenz,Birgit, Napoli,Pietro Emanuele, Galantuomo,Maria Silvana, Fossarello,Maurizio, Cuccu,Alberto, Farci,Roberta, Preising,Markus N, Lorenz,Birgit, and Napoli,Pietro Emanuele

Abstract

Maria Silvana Galantuomo,1,* Maurizio Fossarello,1 Alberto Cuccu,1 Roberta Farci,1 Markus N Preising,2 Birgit Lorenz,2 Pietro Emanuele Napoli1,* 1Department of Surgical Sciences, Eye Clinic, University of Cagliari, Cagliari, Italy; 2Department of Ophthalmology, Faculty of Medicine, Justus-Liebig-University, Giessen, Germany *These authors contributed equally to this work Background: Juvenile X-linked retinoschisis (RS1, OMIM: 312700) is a hereditary vitreoretinal dystrophy characterized by bilateral foveal schisis and, in half of the patients, splitting through the nerve fiber layer in the peripheral retina. In the first decade of life, patients usually develop a decrease in visual acuity. Long-term visual outcomes can be poor due to the limited number of known successful treatments. Purpose: The purposes of this study were to present, for the first time, a p.Arg197Cys missense mutation in the RS1 gene (OMIM: 300839) in a four-generation Italian family with RS1 and to examine the clinical response to the treatment with acetazolamide tablets alone or in combination with dorzolamide eye drops as assessed by spectral-domain optical coherence tomography (SD-OCT). Methods: Eleven individuals, including two brothers with RS1 (patients 1 and 2), underwent a full medical history examination and a comprehensive ocular assessment that involved SD-OCT, fluorescein angiography, electroretinography and DNA analysis. Each RS1 patient received oral acetazolamide (375 mg daily) during the first three months. Thereafter, patient 1 continued only with dorzolamide eyedrops three times a day for a period of three months, while patient 2 spontaneously stopped both medications. Results: Sequence analysis of the RS1 gene identified a hemizygous c.589C>T (p.Arg197Cys) missense mutation in exon 6, which has not been previously reported in an Italian family. A different response to the medical therapy was observed in the four eyes of the two affected brothers hemizygous for this abnor

Published

2016

41. Clinical utility gene card for:Oculocutaneous albinism

Author

Grønskov, Karen, Brøndum-Nielsen, Karen, Lorenz, Birgit, Preising, Markus N, Grønskov, Karen, Brøndum-Nielsen, Karen, Lorenz, Birgit, and Preising, Markus N

Published

2014

42. Clinical utility gene card for:Oculocutaneous albinism

Author

Grønskov, Karen, Brøndum-Nielsen, Karen, Lorenz, Birgit, Preising, Markus N, Grønskov, Karen, Brøndum-Nielsen, Karen, Lorenz, Birgit, and Preising, Markus N

Published

2014

43. Screening of a Large Cohort of Leber Congenital Amaurosis and Retinitis Pigmentosa Patients Identifies Novel LCA5 Mutations and New Genotype-Phenotype Correlations

Author

Mackay, Donna S, Borman, Arundhati Dev, Sui, Ruifang, van den Born, L Ingeborgh, Berson, Eliot L, Ocaka, Louise A, Davidson, Alice E, Heckenlively, John R, Branham, Kari, Ren, Huanan, Lopez, Irma, Maria, Maleeha, Azam, Maleeha, Henkes, Arjen, Blokland, Ellen, Andreasson, Sten, de Baere, Elfride, Bennett, Jean, Chader, Gerald J, Berger, Wolfgang, Golovleva, Irina, Greenberg, Jacquie, den Hollander, Anneke I, Klaver, Caroline C W, Klevering, B Jeroen, Lorenz, Birgit, Preising, Markus N, Ramsear, Raj, Roberts, Lisa, Roepman, Ronald, Rohrschneider, Klaus, Wissinger, Bernd, Qamar, Raheel, Webster, Andrew R, Cremers, Frans P M, Moore, Anthony T, Koenekoop, Robert K, Mackay, Donna S, Borman, Arundhati Dev, Sui, Ruifang, van den Born, L Ingeborgh, Berson, Eliot L, Ocaka, Louise A, Davidson, Alice E, Heckenlively, John R, Branham, Kari, Ren, Huanan, Lopez, Irma, Maria, Maleeha, Azam, Maleeha, Henkes, Arjen, Blokland, Ellen, Andreasson, Sten, de Baere, Elfride, Bennett, Jean, Chader, Gerald J, Berger, Wolfgang, Golovleva, Irina, Greenberg, Jacquie, den Hollander, Anneke I, Klaver, Caroline C W, Klevering, B Jeroen, Lorenz, Birgit, Preising, Markus N, Ramsear, Raj, Roberts, Lisa, Roepman, Ronald, Rohrschneider, Klaus, Wissinger, Bernd, Qamar, Raheel, Webster, Andrew R, Cremers, Frans P M, Moore, Anthony T, and Koenekoop, Robert K

Abstract

This study was undertaken to investigate the prevalence of sequence variants in LCA5 in patients with Leber congenital amaurosis (LCA), early-onset retinal dystrophy (EORD), and autosomal recessive retinitis pigmentosa (arRP); to delineate the ocular phenotypes; and to provide an overview of all published LCA5 variants in an online database. Patients underwent standard ophthalmic evaluations after providing informed consent. In selected patients, optical coherence tomography (OCT) and fundus autofluorescence imaging were possible. DNA samples from 797 unrelated patients with LCA and 211 with the various types of retinitis pigmentosa (RP) were screened by Sanger sequence analysis of all LCA5 exons and intron/exon junctions. Some LCA patients were prescreened by APEX technology or selected based on homozygosity mapping. In silico analyses were performed to assess the pathogenicity of the variants. Segregation analysis was performed where possible. Published and novel LCA5 variants were collected, amended for their correct nomenclature, and listed in a Leiden Open Variation Database (LOVD). Sequence analysis identified 18 new probands with 19 different LCA5 variants. Seventeen of the 19 LCA5 variants were novel. Except for two missense variants and one splice site variant, all variants were protein-truncating mutations. Most patients expressed a severe phenotype, typical of LCA. However, some LCA subjects had better vision and intact inner segment/outer segment (IS/OS) junctions on OCT imaging. In two families with LCA5 variants, the phenotype was more compatible with EORD with affected individuals displaying preserved islands of retinal pigment epithelium. One of the families with a milder phenotype harbored a homozygous splice site mutation; a second family was found to have a combination of a stop mutation and a missense mutation. This is the largest LCA5 study to date. We sequenced 1,008 patients (797 with LCA, 211 with arRP) and identified 18 probands with LCA5 mu

Published

2013

44. Increasing the Yield in Targeted Next-Generation Sequencing by Implicating CNV Analysis, Non-Coding Exons and the Overall Variant Load: The Example of Retinal Dystrophies

Author

Eisenberger, Tobias, Neuhaus, Christine, Khan, Arif O., Decker, Christian, Preising, Markus N., Friedburg, Christoph, Bieg, Anika, Gliem, Martin, Issa, Peter Charbel, Holz, Frank G., Baig, Shahid M., Hellenbroich, Yorck, Galvez, Alberto, Platzer, Konrad, Wollnik, Bernd, Laddach, Nadja, Ghaffari, Saeed Reza, Rafati, Maryam, Botzenhart, Elke, Tinschert, Sigrid, Boerger, Doris, Bohring, Axel, Schreml, Julia, Koertge-Jung, Stefani, Schell-Apacik, Chayim, Bakur, Khadijah, Al-Aama, Jumana Y., Neuhann, Teresa, Herkenrath, Peter, Nuernberg, Gudrun, Nuernburg, Peter, Davis, John S., Gal, Andreas, Bergmann, Carsten, Lorenz, Birgit, Bolz, Hanno J., Eisenberger, Tobias, Neuhaus, Christine, Khan, Arif O., Decker, Christian, Preising, Markus N., Friedburg, Christoph, Bieg, Anika, Gliem, Martin, Issa, Peter Charbel, Holz, Frank G., Baig, Shahid M., Hellenbroich, Yorck, Galvez, Alberto, Platzer, Konrad, Wollnik, Bernd, Laddach, Nadja, Ghaffari, Saeed Reza, Rafati, Maryam, Botzenhart, Elke, Tinschert, Sigrid, Boerger, Doris, Bohring, Axel, Schreml, Julia, Koertge-Jung, Stefani, Schell-Apacik, Chayim, Bakur, Khadijah, Al-Aama, Jumana Y., Neuhann, Teresa, Herkenrath, Peter, Nuernberg, Gudrun, Nuernburg, Peter, Davis, John S., Gal, Andreas, Bergmann, Carsten, Lorenz, Birgit, and Bolz, Hanno J.

Abstract

Retinitis pigmentosa (RP) and Leber congenital amaurosis (LCA) are major causes of blindness. They result from mutations in many genes which has long hampered comprehensive genetic analysis. Recently, targeted next-generation sequencing (NGS) has proven useful to overcome this limitation. To uncover hidden mutations such as copy number variations (CNVs) and mutations in non-coding regions, we extended the use of NGS data by quantitative readout for the exons of 55 RP and LCA genes in 126 patients, and by including non-coding 59 exons. We detected several causative CNVs which were key to the diagnosis in hitherto unsolved constellations, e. g. hemizygous point mutations in consanguineous families, and CNVs complemented apparently monoallelic recessive alleles. Mutations of non-coding exon 1 of EYS revealed its contribution to disease. In view of the high carrier frequency for retinal disease gene mutations in the general population, we considered the overall variant load in each patient to assess if a mutation was causative or reflected accidental carriership in patients with mutations in several genes or with single recessive alleles. For example, truncating mutations in RP1, a gene implicated in both recessive and dominant RP, were causative in biallelic constellations, unrelated to disease when heterozygous on a biallelic mutation background of another gene, or even non-pathogenic if close to the C-terminus. Patients with mutations in several loci were common, but without evidence for di- or oligogenic inheritance. Although the number of targeted genes was low compared to previous studies, the mutation detection rate was highest (70%) which likely results from completeness and depth of coverage, and quantitative data analysis. CNV analysis should routinely be applied in targeted NGS, and mutations in non-coding exons give reason to systematically include 5'-UTRs in disease gene or exome panels. Consideration of all variants is indispensable because even truncating

Published

2013

45. Screening of a large cohort of leber congenital amaurosis and retinitis pigmentosa patients identifies novel LCA5 mutations and new genotype-phenotype correlations.

Author

Mackay, Donna S, Mackay, Donna S, Borman, Arundhati Dev, Sui, Ruifang, van den Born, L Ingeborgh, Berson, Eliot L, Ocaka, Louise A, Davidson, Alice E, Heckenlively, John R, Branham, Kari, Ren, Huanan, Lopez, Irma, Maria, Maleeha, Azam, Maleeha, Henkes, Arjen, Blokland, Ellen, Qamar, Raheel, Webster, Andrew R, Cremers, Frans PM, Moore, Anthony T, Koenekoop, Robert K, [LCA5 Study Group (see acknowledgements for Universities), Andreasson, Sten, de Baere, Elfride, Bennett, Jean, Chader, Gerald J, Berger, Wolfgang, Golovleva, Irina, Greenberg, Jacquie, den Hollander, Anneke I, Klaver, Caroline CW, Klevering, B Jeroen, Lorenz, Birgit, Preising, Markus N, Ramsear, Raj, Roberts, Lisa, Roepman, Ronald, Rohrschneider, Klaus, Wissinger, Bernd, Mackay, Donna S, Mackay, Donna S, Borman, Arundhati Dev, Sui, Ruifang, van den Born, L Ingeborgh, Berson, Eliot L, Ocaka, Louise A, Davidson, Alice E, Heckenlively, John R, Branham, Kari, Ren, Huanan, Lopez, Irma, Maria, Maleeha, Azam, Maleeha, Henkes, Arjen, Blokland, Ellen, Qamar, Raheel, Webster, Andrew R, Cremers, Frans PM, Moore, Anthony T, Koenekoop, Robert K, [LCA5 Study Group (see acknowledgements for Universities), Andreasson, Sten, de Baere, Elfride, Bennett, Jean, Chader, Gerald J, Berger, Wolfgang, Golovleva, Irina, Greenberg, Jacquie, den Hollander, Anneke I, Klaver, Caroline CW, Klevering, B Jeroen, Lorenz, Birgit, Preising, Markus N, Ramsear, Raj, Roberts, Lisa, Roepman, Ronald, Rohrschneider, Klaus, and Wissinger, Bernd

Abstract

This study was undertaken to investigate the prevalence of sequence variants in LCA5 in patients with Leber congenital amaurosis (LCA), early-onset retinal dystrophy (EORD), and autosomal recessive retinitis pigmentosa (arRP); to delineate the ocular phenotypes; and to provide an overview of all published LCA5 variants in an online database. Patients underwent standard ophthalmic evaluations after providing informed consent. In selected patients, optical coherence tomography (OCT) and fundus autofluorescence imaging were possible. DNA samples from 797 unrelated patients with LCA and 211 with the various types of retinitis pigmentosa (RP) were screened by Sanger sequence analysis of all LCA5 exons and intron/exon junctions. Some LCA patients were prescreened by APEX technology or selected based on homozygosity mapping. In silico analyses were performed to assess the pathogenicity of the variants. Segregation analysis was performed where possible. Published and novel LCA5 variants were collected, amended for their correct nomenclature, and listed in a Leiden Open Variation Database (LOVD). Sequence analysis identified 18 new probands with 19 different LCA5 variants. Seventeen of the 19 LCA5 variants were novel. Except for two missense variants and one splice site variant, all variants were protein-truncating mutations. Most patients expressed a severe phenotype, typical of LCA. However, some LCA subjects had better vision and intact inner segment/outer segment (IS/OS) junctions on OCT imaging. In two families with LCA5 variants, the phenotype was more compatible with EORD with affected individuals displaying preserved islands of retinal pigment epithelium. One of the families with a milder phenotype harbored a homozygous splice site mutation; a second family was found to have a combination of a stop mutation and a missense mutation. This is the largest LCA5 study to date. We sequenced 1,008 patients (797 with LCA, 211 with arRP) and identified 18 probands with LCA5 mu

Published

2013

46. Increasing the Yield in Targeted Next-Generation Sequencing by Implicating CNV Analysis, Non-Coding Exons and the Overall Variant Load: The Example of Retinal Dystrophies

Author

Eisenberger, Tobias, Neuhaus, Christine, Khan, Arif O., Decker, Christian, Preising, Markus N., Friedburg, Christoph, Bieg, Anika, Gliem, Martin, Issa, Peter Charbel, Holz, Frank G., Baig, Shahid M., Hellenbroich, Yorck, Galvez, Alberto, Platzer, Konrad, Wollnik, Bernd, Laddach, Nadja, Ghaffari, Saeed Reza, Rafati, Maryam, Botzenhart, Elke, Tinschert, Sigrid, Boerger, Doris, Bohring, Axel, Schreml, Julia, Koertge-Jung, Stefani, Schell-Apacik, Chayim, Bakur, Khadijah, Al-Aama, Jumana Y., Neuhann, Teresa, Herkenrath, Peter, Nuernberg, Gudrun, Nuernburg, Peter, Davis, John S., Gal, Andreas, Bergmann, Carsten, Lorenz, Birgit, Bolz, Hanno J., Eisenberger, Tobias, Neuhaus, Christine, Khan, Arif O., Decker, Christian, Preising, Markus N., Friedburg, Christoph, Bieg, Anika, Gliem, Martin, Issa, Peter Charbel, Holz, Frank G., Baig, Shahid M., Hellenbroich, Yorck, Galvez, Alberto, Platzer, Konrad, Wollnik, Bernd, Laddach, Nadja, Ghaffari, Saeed Reza, Rafati, Maryam, Botzenhart, Elke, Tinschert, Sigrid, Boerger, Doris, Bohring, Axel, Schreml, Julia, Koertge-Jung, Stefani, Schell-Apacik, Chayim, Bakur, Khadijah, Al-Aama, Jumana Y., Neuhann, Teresa, Herkenrath, Peter, Nuernberg, Gudrun, Nuernburg, Peter, Davis, John S., Gal, Andreas, Bergmann, Carsten, Lorenz, Birgit, and Bolz, Hanno J.

Abstract

Retinitis pigmentosa (RP) and Leber congenital amaurosis (LCA) are major causes of blindness. They result from mutations in many genes which has long hampered comprehensive genetic analysis. Recently, targeted next-generation sequencing (NGS) has proven useful to overcome this limitation. To uncover hidden mutations such as copy number variations (CNVs) and mutations in non-coding regions, we extended the use of NGS data by quantitative readout for the exons of 55 RP and LCA genes in 126 patients, and by including non-coding 59 exons. We detected several causative CNVs which were key to the diagnosis in hitherto unsolved constellations, e. g. hemizygous point mutations in consanguineous families, and CNVs complemented apparently monoallelic recessive alleles. Mutations of non-coding exon 1 of EYS revealed its contribution to disease. In view of the high carrier frequency for retinal disease gene mutations in the general population, we considered the overall variant load in each patient to assess if a mutation was causative or reflected accidental carriership in patients with mutations in several genes or with single recessive alleles. For example, truncating mutations in RP1, a gene implicated in both recessive and dominant RP, were causative in biallelic constellations, unrelated to disease when heterozygous on a biallelic mutation background of another gene, or even non-pathogenic if close to the C-terminus. Patients with mutations in several loci were common, but without evidence for di- or oligogenic inheritance. Although the number of targeted genes was low compared to previous studies, the mutation detection rate was highest (70%) which likely results from completeness and depth of coverage, and quantitative data analysis. CNV analysis should routinely be applied in targeted NGS, and mutations in non-coding exons give reason to systematically include 5'-UTRs in disease gene or exome panels. Consideration of all variants is indispensable because even truncating

Published

2013

47. Prevalence and Diagnostic Spectrum of Generalized Retinal Dystrophy in Danish Children

Author

Bertelsen, Mette, Jensen, Hanne, Larsen, Michael, Lorenz, Birgit, Preising, Markus N, Rosenberg, Thomas, Bertelsen, Mette, Jensen, Hanne, Larsen, Michael, Lorenz, Birgit, Preising, Markus N, and Rosenberg, Thomas

Abstract

Purpose: The aim of the present population-based cross-sectional study was to examine the prevalence and diagnostic spectrum of generalized retinal dystrophy in Danish children. Methods: The Danish Registry for the Blind and Partially Sighted Children comprises all visually impaired children residing in Denmark aged 0-17 years. Among registered children, the primary diagnosis of generalized retinal dystrophy was assessed by chart review, including fundus photographs and electroretinograms. Age-specific data for live children in Denmark were retrieved from Statistics Denmark. Results: Of the 1,204,235 Danish children aged 0-17 years on 1 October 2011, 2017 children were registered as visually impaired. Of these, 153 cases were attributed to generalized retinal dystrophy, corresponding to a prevalence of 13 per 100,000 children. The age-specific prevalence increased prominently with increasing age. In 43% of the children the eye condition was part of a syndrome, while the remaining 57% had eye disease only. The most common hereditary pattern was autosomal recessive (99 children, 66%). Conclusions: This epidemiological survey demonstrates that the prevalence of generalized retinal dystrophy in Danish children is 13 per 100,000, which is a considerable increase compared to the 9.8 per 100,000 reported by Rosenberg in 1988. The prevalence of Leber congenital amaurosis, Usher syndrome, and Bardet-Biedl syndrome doubled, which may be explained by a documented history of consanguinity in more than one third of the children. Many of the dystrophies are the subject of clinical intervention trials, and nation-wide epidemiological data can help assess the future need for treatment.

Published

2013

48. Prevalence and Diagnostic Spectrum of Generalized Retinal Dystrophy in Danish Children

Author

Bertelsen, Mette, Jensen, Hanne, Larsen, Michael, Lorenz, Birgit, Preising, Markus N, Rosenberg, Thomas, Bertelsen, Mette, Jensen, Hanne, Larsen, Michael, Lorenz, Birgit, Preising, Markus N, and Rosenberg, Thomas

Abstract

Purpose: The aim of the present population-based cross-sectional study was to examine the prevalence and diagnostic spectrum of generalized retinal dystrophy in Danish children. Methods: The Danish Registry for the Blind and Partially Sighted Children comprises all visually impaired children residing in Denmark aged 0-17 years. Among registered children, the primary diagnosis of generalized retinal dystrophy was assessed by chart review, including fundus photographs and electroretinograms. Age-specific data for live children in Denmark were retrieved from Statistics Denmark. Results: Of the 1,204,235 Danish children aged 0-17 years on 1 October 2011, 2017 children were registered as visually impaired. Of these, 153 cases were attributed to generalized retinal dystrophy, corresponding to a prevalence of 13 per 100,000 children. The age-specific prevalence increased prominently with increasing age. In 43% of the children the eye condition was part of a syndrome, while the remaining 57% had eye disease only. The most common hereditary pattern was autosomal recessive (99 children, 66%). Conclusions: This epidemiological survey demonstrates that the prevalence of generalized retinal dystrophy in Danish children is 13 per 100,000, which is a considerable increase compared to the 9.8 per 100,000 reported by Rosenberg in 1988. The prevalence of Leber congenital amaurosis, Usher syndrome, and Bardet-Biedl syndrome doubled, which may be explained by a documented history of consanguinity in more than one third of the children. Many of the dystrophies are the subject of clinical intervention trials, and nation-wide epidemiological data can help assess the future need for treatment.

Published

2013

49. Fundus albipunctatus associated with compound heterozygous mutations in RPE65

Author

Schatz, Patrik, Preising, Markus, Lorenz, Birgit, Sander, Birgit, Larsen, Michael, Rosenberg, Thomas, Schatz, Patrik, Preising, Markus, Lorenz, Birgit, Sander, Birgit, Larsen, Michael, and Rosenberg, Thomas

Abstract

To describe a family with an 18-year-old woman with fundus albipunctatus and compound heterozygous mutations in RPE65 whose unaffected parents and 1 female sibling harbored single heterozygous RPE65 mutations.

Published

2011

50. Fundus albipunctatus associated with compound heterozygous mutations in RPE65

Author

Schatz, Patrik, Preising, Markus, Lorenz, Birgit, Sander, Birgit, Larsen, Michael, Rosenberg, Thomas, Schatz, Patrik, Preising, Markus, Lorenz, Birgit, Sander, Birgit, Larsen, Michael, and Rosenberg, Thomas

Abstract

To describe a family with an 18-year-old woman with fundus albipunctatus and compound heterozygous mutations in RPE65 whose unaffected parents and 1 female sibling harbored single heterozygous RPE65 mutations.

Published

2011