RPGR-Related Retinal Dystrophy in Latin America—A Collaborative Study

Malena Daich Varela; Rene Moya; José D. Luna; Marcela Ciccioli; M. Eugenia Inga; Julieta Gras; Pedro J. Nuova; Luciana Capalbo; Alejandra Antacle; Laura Echandi; Angelica Moussali; Alejandro Sanders Villa; Marcela Pérez Araya; Tamara Muhlberger; Rocio A. Villafuerte-de la Cruz; Adda Villanueva; Tania Barragán Arévalo; Olivia Araujo Zin; Thiago Carvalho Barros de Oliveira; Fernanda Belga Ottoni Porto; Gustavo Barreto de Melo; Caio Henrique Marques Texeira; Mariana Vallim Salles; Renata Moreto; Jose Ronaldo Lima de Carvalho; Mariana Matioli da Palma; Rebeca Azevedo Souza Amaral; Cecília Francini Cabral de Vasconcellos; Gabriela Doná Rodrigues; Rosane Guazi Resende; Fabiana Louise Teixeira Motta; Luiz Alexandre Rassi Gabriel; Debora Moraes; Nancy Gelvez; Greizy López; Martha L. Tamayo; Juliana Maria Ferraz Sallum

RPGR-Related Retinal Dystrophy in Latin America—A Collaborative Study

Malena Daich Varela, Rene Moya, José D. Luna, Marcela Ciccioli, M. Eugenia Inga, Julieta Gras, Pedro J. Nuova, Luciana Capalbo, Alejandra Antacle, Laura Echandi, Angelica Moussali, Alejandro Sanders Villa, Marcela Pérez Araya, Tamara Muhlberger, Rocio A. Villafuerte-de la Cruz, Adda Villanueva, Tania Barragán Arévalo, Olivia Araujo Zin, Thiago Carvalho Barros de Oliveira, Fernanda Belga Ottoni PortoGustavo Barreto de Melo, Caio Henrique Marques Texeira, Mariana Vallim Salles, Renata Moreto, Jose Ronaldo Lima de Carvalho, Mariana Matioli da Palma, Rebeca Azevedo Souza Amaral, Cecília Francini Cabral de Vasconcellos, Gabriela Doná Rodrigues, Rosane Guazi Resende, Fabiana Louise Teixeira Motta, Luiz Alexandre Rassi Gabriel, Debora Moraes, Nancy Gelvez, Greizy López, Martha L. Tamayo, Juliana Maria Ferraz Sallum

Instituto de Genética Humana

Producción: Contribución a una revista › Artículo › revisión exhaustiva

Resumen

Purpose: To provide the first genetic and clinical characterization of RPGR-associated inherited retinal diseases (IRDs) in Latin America and assess their genetic, clinical, and socioeconomic landscape. Design: Multicenter, international, retrospective, observational cohort study. Methods: Patients with genetically confirmed RPGR-IRD from Brazil, Argentina, Chile, Mexico, Colombia, and Panama were included in this study. Demographic, clinical, genetic, and socioeconomic data were collected and analyzed to characterize disease prevalence and severity, assess rate of progression, and draw genotype-phenotype correlations. A socioeconomic evaluation analyzed healthcare costs and employment. Results: The study describes the largest cohort to date of patients with RPGR-associated IRD, with 314 individuals from 205 families carrying likely disease-causing variants. Of these, 276 individuals (88%) had retinitis pigmentosa, with a mean age of disease onset at 10.9 ± 7.6 years. Analyzed cross-sectionally at the baseline visit (age 27.3 ± 17.2 years), there was a statistically significant association between age and best-corrected visual acuity (BCVA, P < .0001, R² = 0.3). Kaplan–Meier analysis showed that more than 90% of patients would maintain binocular BCVA better than 1.0 logMAR until age 40 years, decreasing to 50% by age 57 years, and by 58 years of age 50% of patients would have discernible subfoveal ellipsoid zone. The mean age of male patients whose BCVA was 1.0 logMAR or worse in their better-seeing eye was 48.3 ± 9.5 years (median, 49 years). Fourteen previously unreported variants in RPGR are described. Among patients who declared employment status (n = 122), 43% reported being unemployed or in part-time employment due to their visual impairment; among those who reported mental health well-being (n = 133), 45% reported depression or anxiety. Conclusions: This study provides the first genetic and clinical characterization of RPGR-IRD in Latin America, contributing previously unreported variants, natural history details, genotype-phenotype correlations, and an estimated regional prevalence. By providing data on potentially eligible patients, their clinical status, and the socioeconomic impact of RPGR-IRDs, this study lays the foundation for potential access to RPGR future therapies in Latin America.

Idioma original	Inglés
Páginas (desde-hasta)	313-322
Número de páginas	10
Publicación	American Journal of Ophthalmology
Volumen	277
Fecha en línea anticipada	27 may. 2025
Estado	Publicada - sep. 2025

ODS de las Naciones Unidas

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Daich Varela, M., Moya, R., Luna, J. D., Ciccioli, M., Inga, M. E., Gras, J., Nuova, P. J., Capalbo, L., Antacle, A., Echandi, L., Moussali, A., Sanders Villa, A., Araya, M. P., Muhlberger, T., Villafuerte-de la Cruz, R. A., Villanueva, A., Arévalo, T. B., Zin, O. A., de Oliveira, T. C. B., ... Sallum, J. M. F. (2025). RPGR-Related Retinal Dystrophy in Latin America—A Collaborative Study. American Journal of Ophthalmology, 277, 313-322.

@article{84f16383596648f495e5cadb8dd54634,

title = "RPGR-Related Retinal Dystrophy in Latin America—A Collaborative Study",

abstract = "Purpose: To provide the first genetic and clinical characterization of RPGR-associated inherited retinal diseases (IRDs) in Latin America and assess their genetic, clinical, and socioeconomic landscape. Design: Multicenter, international, retrospective, observational cohort study. Methods: Patients with genetically confirmed RPGR-IRD from Brazil, Argentina, Chile, Mexico, Colombia, and Panama were included in this study. Demographic, clinical, genetic, and socioeconomic data were collected and analyzed to characterize disease prevalence and severity, assess rate of progression, and draw genotype-phenotype correlations. A socioeconomic evaluation analyzed healthcare costs and employment. Results: The study describes the largest cohort to date of patients with RPGR-associated IRD, with 314 individuals from 205 families carrying likely disease-causing variants. Of these, 276 individuals (88\%) had retinitis pigmentosa, with a mean age of disease onset at 10.9 ± 7.6 years. Analyzed cross-sectionally at the baseline visit (age 27.3 ± 17.2 years), there was a statistically significant association between age and best-corrected visual acuity (BCVA, P < .0001, R2 = 0.3). Kaplan–Meier analysis showed that more than 90\% of patients would maintain binocular BCVA better than 1.0 logMAR until age 40 years, decreasing to 50\% by age 57 years, and by 58 years of age 50\% of patients would have discernible subfoveal ellipsoid zone. The mean age of male patients whose BCVA was 1.0 logMAR or worse in their better-seeing eye was 48.3 ± 9.5 years (median, 49 years). Fourteen previously unreported variants in RPGR are described. Among patients who declared employment status (n = 122), 43\% reported being unemployed or in part-time employment due to their visual impairment; among those who reported mental health well-being (n = 133), 45\% reported depression or anxiety. Conclusions: This study provides the first genetic and clinical characterization of RPGR-IRD in Latin America, contributing previously unreported variants, natural history details, genotype-phenotype correlations, and an estimated regional prevalence. By providing data on potentially eligible patients, their clinical status, and the socioeconomic impact of RPGR-IRDs, this study lays the foundation for potential access to RPGR future therapies in Latin America.",

author = "\{Daich Varela\}, Malena and Rene Moya and Luna, \{Jos{\'e} D.\} and Marcela Ciccioli and Inga, \{M. Eugenia\} and Julieta Gras and Nuova, \{Pedro J.\} and Luciana Capalbo and Alejandra Antacle and Laura Echandi and Angelica Moussali and \{Sanders Villa\}, Alejandro and Araya, \{Marcela P{\'e}rez\} and Tamara Muhlberger and \{Villafuerte-de la Cruz\}, \{Rocio A.\} and Adda Villanueva and Ar{\'e}valo, \{Tania Barrag{\'a}n\} and Zin, \{Olivia Araujo\} and \{de Oliveira\}, \{Thiago Carvalho Barros\} and Porto, \{Fernanda Belga Ottoni\} and \{de Melo\}, \{Gustavo Barreto\} and Texeira, \{Caio Henrique Marques\} and Salles, \{Mariana Vallim\} and Renata Moreto and \{de Carvalho\}, \{Jose Ronaldo Lima\} and \{da Palma\}, \{Mariana Matioli\} and Amaral, \{Rebeca Azevedo Souza\} and \{de Vasconcellos\}, \{Cec{\'i}lia Francini Cabral\} and Rodrigues, \{Gabriela Don{\'a}\} and Resende, \{Rosane Guazi\} and Motta, \{Fabiana Louise Teixeira\} and Gabriel, \{Luiz Alexandre Rassi\} and Debora Moraes and Nancy Gelvez and Greizy L{\'o}pez and Tamayo, \{Martha L.\} and Sallum, \{Juliana Maria Ferraz\}",

year = "2025",

month = sep,

language = "English",

volume = "277",

pages = "313--322",

journal = "American Journal of Ophthalmology",

issn = "0002-9394",

publisher = "Elsevier Inc.",

}

Daich Varela, M, Moya, R, Luna, JD, Ciccioli, M, Inga, ME, Gras, J, Nuova, PJ, Capalbo, L, Antacle, A, Echandi, L, Moussali, A, Sanders Villa, A, Araya, MP, Muhlberger, T, Villafuerte-de la Cruz, RA, Villanueva, A, Arévalo, TB, Zin, OA, de Oliveira, TCB, Porto, FBO, de Melo, GB, Texeira, CHM, Salles, MV, Moreto, R, de Carvalho, JRL, da Palma, MM, Amaral, RAS, de Vasconcellos, CFC, Rodrigues, GD, Resende, RG, Motta, FLT, Gabriel, LAR, Moraes, D, Gelvez, N , López, G , Tamayo, ML & Sallum, JMF 2025, 'RPGR-Related Retinal Dystrophy in Latin America—A Collaborative Study', American Journal of Ophthalmology, vol. 277, pp. 313-322.

TY - JOUR

T1 - RPGR-Related Retinal Dystrophy in Latin America—A Collaborative Study

AU - Daich Varela, Malena

AU - Moya, Rene

AU - Luna, José D.

AU - Ciccioli, Marcela

AU - Inga, M. Eugenia

AU - Gras, Julieta

AU - Nuova, Pedro J.

AU - Capalbo, Luciana

AU - Antacle, Alejandra

AU - Echandi, Laura

AU - Moussali, Angelica

AU - Sanders Villa, Alejandro

AU - Araya, Marcela Pérez

AU - Muhlberger, Tamara

AU - Villafuerte-de la Cruz, Rocio A.

AU - Villanueva, Adda

AU - Arévalo, Tania Barragán

AU - Zin, Olivia Araujo

AU - de Oliveira, Thiago Carvalho Barros

AU - Porto, Fernanda Belga Ottoni

AU - de Melo, Gustavo Barreto

AU - Texeira, Caio Henrique Marques

AU - Salles, Mariana Vallim

AU - Moreto, Renata

AU - de Carvalho, Jose Ronaldo Lima

AU - da Palma, Mariana Matioli

AU - Amaral, Rebeca Azevedo Souza

AU - de Vasconcellos, Cecília Francini Cabral

AU - Rodrigues, Gabriela Doná

AU - Resende, Rosane Guazi

AU - Motta, Fabiana Louise Teixeira

AU - Gabriel, Luiz Alexandre Rassi

AU - Moraes, Debora

AU - Gelvez, Nancy

AU - López, Greizy

AU - Tamayo, Martha L.

AU - Sallum, Juliana Maria Ferraz

PY - 2025/9

Y1 - 2025/9

N2 - Purpose: To provide the first genetic and clinical characterization of RPGR-associated inherited retinal diseases (IRDs) in Latin America and assess their genetic, clinical, and socioeconomic landscape. Design: Multicenter, international, retrospective, observational cohort study. Methods: Patients with genetically confirmed RPGR-IRD from Brazil, Argentina, Chile, Mexico, Colombia, and Panama were included in this study. Demographic, clinical, genetic, and socioeconomic data were collected and analyzed to characterize disease prevalence and severity, assess rate of progression, and draw genotype-phenotype correlations. A socioeconomic evaluation analyzed healthcare costs and employment. Results: The study describes the largest cohort to date of patients with RPGR-associated IRD, with 314 individuals from 205 families carrying likely disease-causing variants. Of these, 276 individuals (88%) had retinitis pigmentosa, with a mean age of disease onset at 10.9 ± 7.6 years. Analyzed cross-sectionally at the baseline visit (age 27.3 ± 17.2 years), there was a statistically significant association between age and best-corrected visual acuity (BCVA, P < .0001, R2 = 0.3). Kaplan–Meier analysis showed that more than 90% of patients would maintain binocular BCVA better than 1.0 logMAR until age 40 years, decreasing to 50% by age 57 years, and by 58 years of age 50% of patients would have discernible subfoveal ellipsoid zone. The mean age of male patients whose BCVA was 1.0 logMAR or worse in their better-seeing eye was 48.3 ± 9.5 years (median, 49 years). Fourteen previously unreported variants in RPGR are described. Among patients who declared employment status (n = 122), 43% reported being unemployed or in part-time employment due to their visual impairment; among those who reported mental health well-being (n = 133), 45% reported depression or anxiety. Conclusions: This study provides the first genetic and clinical characterization of RPGR-IRD in Latin America, contributing previously unreported variants, natural history details, genotype-phenotype correlations, and an estimated regional prevalence. By providing data on potentially eligible patients, their clinical status, and the socioeconomic impact of RPGR-IRDs, this study lays the foundation for potential access to RPGR future therapies in Latin America.

AB - Purpose: To provide the first genetic and clinical characterization of RPGR-associated inherited retinal diseases (IRDs) in Latin America and assess their genetic, clinical, and socioeconomic landscape. Design: Multicenter, international, retrospective, observational cohort study. Methods: Patients with genetically confirmed RPGR-IRD from Brazil, Argentina, Chile, Mexico, Colombia, and Panama were included in this study. Demographic, clinical, genetic, and socioeconomic data were collected and analyzed to characterize disease prevalence and severity, assess rate of progression, and draw genotype-phenotype correlations. A socioeconomic evaluation analyzed healthcare costs and employment. Results: The study describes the largest cohort to date of patients with RPGR-associated IRD, with 314 individuals from 205 families carrying likely disease-causing variants. Of these, 276 individuals (88%) had retinitis pigmentosa, with a mean age of disease onset at 10.9 ± 7.6 years. Analyzed cross-sectionally at the baseline visit (age 27.3 ± 17.2 years), there was a statistically significant association between age and best-corrected visual acuity (BCVA, P < .0001, R2 = 0.3). Kaplan–Meier analysis showed that more than 90% of patients would maintain binocular BCVA better than 1.0 logMAR until age 40 years, decreasing to 50% by age 57 years, and by 58 years of age 50% of patients would have discernible subfoveal ellipsoid zone. The mean age of male patients whose BCVA was 1.0 logMAR or worse in their better-seeing eye was 48.3 ± 9.5 years (median, 49 years). Fourteen previously unreported variants in RPGR are described. Among patients who declared employment status (n = 122), 43% reported being unemployed or in part-time employment due to their visual impairment; among those who reported mental health well-being (n = 133), 45% reported depression or anxiety. Conclusions: This study provides the first genetic and clinical characterization of RPGR-IRD in Latin America, contributing previously unreported variants, natural history details, genotype-phenotype correlations, and an estimated regional prevalence. By providing data on potentially eligible patients, their clinical status, and the socioeconomic impact of RPGR-IRDs, this study lays the foundation for potential access to RPGR future therapies in Latin America.

UR - https://www.scopus.com/pages/publications/105008565346

UR - https://www.mendeley.com/catalogue/2b9e0a9c-d594-304e-8e61-9d84dbfcd279/

M3 - Article

C2 - 40441500

SN - 0002-9394

VL - 277

SP - 313

EP - 322

JO - American Journal of Ophthalmology

JF - American Journal of Ophthalmology

ER -

RPGR-Related Retinal Dystrophy in Latin America—A Collaborative Study

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