Your search keyword '"Mazzetti, Pilar"' showing total 8 results

1. Neurogenetics in Peru: clinical, scientific and ethical perspectives

Author

Cornejo-Olivas, Mario, Espinoza-Huertas, Keren, Velit-Salazar, Mario R., Veliz-Otani, Diego, Tirado-Hurtado, Indira, Inca-Martinez, Miguel, Silva-Paredes, Gustavo, Milla-Neyra, Karina, Marca, Victoria, Ortega, Olimpio, and Mazzetti, Pilar

Published

2015

2. Juvenile‐Onset Huntington's Disease in Peru: A Case Series of 32 Patients.

Author

Vishnevetsky, Anastasia, Cornejo‐Olivas, Mario, Sarapura‐Castro, Elison, Inca‐Martinez, Miguel, Rabinowitz, Danielle, Milla‐Neyra, Karina, Mazzetti, Pilar, and Bird, Thomas

Subjects

HUNTINGTON disease, JUVENILE diseases, SLEEP interruptions, AGE of onset, DATABASES

Abstract

Background: Juvenile‐onset Huntington's Disease (JoHD) or Huntington's disease (HD) with age of onset ≤20 years, is a rare clinical entity that often differs phenotypically from adult HD and represents only 1–15% of total HD cases. Objective: To characterize the genetic and clinical characteristics of 32 JoHD patients seen in a Peruvian Neurogenetics clinic from 2000–2018. Methods: This study is a retrospective clinical and genetic review. The clinical database in Lima, Peru was searched for HD patients seen in clinic between 2000 and 2018. Inclusion criteria were: (1) genetically confirmed disease; and (2) HD age of onset ≤20 years, according to the documented medical history. Results: Among 475 patients with genetically confirmed HD in the database, 32 patients (6.7%) had symptom onset at ≤20 years. Among JoHD patients with a known transmitting parent (30 of 32), paternal transmission accounted for 77% of cases. Anticipation was higher with paternal transmission compared to maternal transmission (27.5 ± 11.5 vs. 11.3 ± 7.1 years). Overall expanded CAG repeat length ranged from 44 to 110, with a mean length of 65.6 ± 15.4, and 14 (44%) cases had repeat length under 60. Of the 32 patients included in the study, 25 had detailed clinical symptomatology available, and many patients had unique clinical features such as prominent sleep disturbance (60% of patients), or parkinsonism (73%). Conclusions: This large case series of JoHD patients characterizes the Peruvian JoHD population, reports on unique familial relationships in JoHD, and highlights the varied symptomatic presentation of this rare disease. [ABSTRACT FROM AUTHOR]

Published

2023

3. Neurogenetics in Peru, example of translational research

Author

Mazzetti, Pilar, Inca-Martínez, Miguel, Tirado-Hurtado, Indira, Milla-Neyra, Karina, Silva-Paredes, Gustavo, Vishnevetsky, Anastasia, and Cornejo-Olivas, Mario

Subjects

investigación traslacional, lcsh:R5-920, Genotype, lcsh:R, lcsh:Medicine, Translational research, Neurology, Genetics, Investigación traslacional, Neurología, Genética, genética, neurología, Translational Research, Biomedical, Peru, Humans, Nervous System Diseases, lcsh:Medicine (General)

Abstract

Neurogenetics is an emerging discipline in Peru that links basic research with clinical practice. The Neurogenetics Research Center located in Lima, Peru is the only unit dedicated to the specialized care of neurogenetic diseases in the country. From the beginning, neurogenetics research has been closely linked to the study of Huntington’s Disease (HD), from the PCRgenotyping of the HTT gene, to the current haplogroup studies in HD. Research in other monogenic diseases led to the implementation of alternative methodologies for the genotyping of Fragile X and Myotonic Dystrophy Type 1. Both, national and international collaborative efforts have facilitated the discovery of new genetic variants in complex multigenic diseasessuch as Parkinson’s disease and Alzheimer’s disease. Additionally, multidisciplinary education and mentoring have allowed for the training of new neurogenetics specialists, supporting the sustained growth of the discipline in the country. The promotion of research in Peru has spurred the growth of neurogenetics research, although limitations in infrastructure, technology, and education remain a challenge for the further growth of research in this field. La neurogenética es una disciplina emergente en el Perú que vincula la investigación básica con la práctica clínica. El Centro de Investigación Básica en Neurogenética, es el único centro en el Perú dedicado a la atención especializada de enfermedades neurogenéticas. La investigación en esta área está estrechamente ligada a la enfermedad de Huntington, desde la genotipificación del gen HTT por PCR, hasta los actuales estudios de haplogrupos en esta enfermedad. La investigación en otras enfermedades monogénicas permitió la implementación de metodologías alternativas para la genotipificación del síndrome X frágil y distrofia miotónica tipo 1. Esfuerzos colaborativos nacionales e internacionales han permitido conocer nuevas variantes genéticas en enfermedades complejas, como la enfermedad de Parkinson y Alzheimer. El entrenamiento multidisciplinario y la mentoría fomentan la formación de nuevos especialistas en neurogenética, permitiendo el crecimiento sostenido de esta disciplina en el país. El impulso de la investigación en el Perú ha impulsado el crecimiento de la investigación en neurogenética; sin embargo, las limitaciones en infraestructura, tecnología y capacitación aún son un reto para el crecimiento de investigación en esta disciplina.

Published

2015

4. Genetic Analysis of Hereditary Ataxias in Peru Identifies SCA10 Families with Incomplete Penetrance.

Author

Cornejo-Olivas, Mario, Inca-Martinez, Miguel, Castilhos, Raphael Machado, Furtado, Gabriel Vasata, Mattos, Eduardo Preusser, Bampi, Giovana Bavia, Leistner-Segal, Sandra, Marca, Victoria, Mazzetti, Pilar, Saraiva-Pereira, Maria Luiza, and Jardim, Laura Bannach

Subjects

FRIEDREICH'S ataxia, NUCLEAR families, FAMILIES, SPINOCEREBELLAR ataxia, ATAXIA, CEREBELLUM degeneration, RECESSIVE genes

Abstract

Relative frequency of hereditary ataxias remains unknown in many regions of Latin America. We described the relative frequency in spinocerebellar ataxias (SCA) due to (CAG)n and to (ATTCT)n expansions, as well as Friedreich ataxia (FRDA), among cases series of ataxic individuals from Peru. Among ataxic index cases from 104 families (38 of them with and 66 without autosomal dominant pattern of inheritance), we identified 22 SCA10, 8 SCA2, 3 SCA6, 2 SCA3, 2 SCA7, 1 SCA1, and 9 FRDA cases (or families). SCA10 was by far the most frequent one. Findings in SCA10 and FRDA families were of note. Affected genitors were not detected in 7 out of 22 SCA10 nuclear families; then overall maximal penetrance of SCA10 was estimated as 85%; in multiplex families, penetrance was 94%. Two out of nine FRDA cases carried only one allele with a GAA expansion. SCA10 was the most frequent hereditary ataxia in Peru. Our data suggested that ATTCT expansions at ATXN10 might not be fully penetrant and/or instability between generations might frequently cross the limits between non-penetrant and penetrant lengths. A unique distribution of inherited ataxias in Peru requires specific screening panels, considering SCA10 as first line of local diagnosis guidelines. [ABSTRACT FROM AUTHOR]

Published

2020

5. Homocystinuria, a metabolic disease of late diagnosis in Peru

Author

Cornejo-Olivas, Mario R, Chávez-Pasco, Vilma G, Inca-Martínez, Miguel A, Véliz-Otani, Diego M, Mora-Alférez, Anali P, Velit-Salazar, Mario R, Sánchez-Boluarte, Arantxa, Quiroga de Michelena, Maria, and Mazzetti, Pilar

Subjects

Enfermedades metabólicas, Perú, Peru, hábito marfanoide, metabolic disorders, Homocystinuria, marphanoid habitus, delayed diagnosis, diagnóstico tardío, homocistinuria

Abstract

La Homocistinuria, es un desorden metabólico autosómico recesivo, cuya forma clásica es causada por deficiencia de cistationina β-sintasa, debido a mutaciones en el gen CBS (Cr21q22.3). Se describe el caso de un varón de 17 años con hipopigmentación de piel y faneras, retraso psicomotor moderado, hábito marfanoide, miopía severa, subluxación del cristalino bilateral, que además presentóeventos psicóticos y una hemiparesia izquierda secundaria a un infartolacunar. La determinación de homocisteína en plasma se encontró elevada (>9,9mg/dl), así como niveles altos denitroprusiato de sodio en orina(4+)que confirmaron el diagnóstico clínico de homocistinuria. La homocistinuria clásica genera múltiples complicaciones a nivel dérmico, oftalmológico, cognitivo, osteoarticular y psiquiátrico; que podrían evitarse con un diagnóstico y tratamiento oportuno a través del tamizaje neonatal, aún no disponible en la mayoría de centros asistenciales en el Perú. Homocystinuria is an autosomal-recessive metabolic disorder whose classical phenotype is caused by a deficiency of cystathionine β-synthase, dueto mutations within the CBS gene(Cr21q22.3). Here in we report a 17 years old man with hypopigmented skin and hair, mental retardation, marfanoid habitus, severe myopia, bilateral lens subluxation, psychotic episodes, and left-sided hemiparesis secondary to alacunar brain infarction. Laboratory tests showed increased levels of homocysteine (>9.9mg/dl) in plasma and high levels of urinary sodium nitroprusside (4+), consistent with the clinical diagnosis of classical homocystinuria. This systemic disorder includes dermal, ophthalmic, cognitive, osteoarticular and psychiatric alterations, all of which could be potentially prevented with early diagnosis and therapy as part of new born screening, which is still unavailable in Peru.

Published

2015

6. Genetics and genomics in Peru: Clinical and research perspective.

Author

Guio, Heinner, Poterico, Julio A., Levano, Kelly S., Cornejo‐Olivas, Mario, Mazzetti, Pilar, Manassero‐Morales, Gioconda, Ugarte‐Gil, Manuel F., Acevedo‐Vásquez, Eduardo, Dueñas‐Roque, Milagros, Piscoya, Alejandro, Fujita, Ricardo, Sanchez, Cesar, Casavilca‐Zambrano, Sandro, Jaramillo‐Valverde, Luis, Sullcahuaman‐Allende, Yasser, Iglesias‐Pedraz, Juan M., and Abarca‐Barriga, Hugo

Subjects

PUBLIC health, TROPICAL medicine, GENETIC polymorphisms, ZIKA virus infections, CLINICAL trials

Abstract

Peruvians currently preserve in their DNA the history of 2.5 million years of human evolution and 150,000 years of migration from Africa to Peru or the Americas. The development of Genetics and Genomics in the clinical and academic field is shown in this review. [ABSTRACT FROM AUTHOR]

Published

2018

7. Clinical and Molecular Features of Late Onset Huntington Disease in a Peruvian Cohort.

Author

Velit-Salazar, Mario R., Mazzetti, Pilar, Cornejo-Olivas, Mario R., Inca-Martinez, Miguel A., Espinoza-Huertas, Keren, Veliz-Otani, Diego, Marca, Victoria, Ortega, Olimpio, Cornejo-Herrera, Ivan F., Lindo-Samanamud, Saul, and Mora-Alferez, Pamela

Subjects

*HUNTINGTON disease, *CHOREA, *AGE of onset, *NUCLEOTIDE sequence, *COHORT analysis, *PATIENTS, *PROGNOSIS

Abstract

Background: Late onset cases of Huntington disease (HD), with onset ≥⃒60 years, account for up to 20% of HD cases worldwide. Clinical features include mild motor dysfunction with slow progression and cognitive impairment, frequent absence of family history and low number of CAG repeats. The clinical and molecular features of late onset HD is still understudied in Latin America. Objectives: To describe the clinical and molecular characteristics of late onset HD in a Peruvian cohort. Methods: An observational study was carried out by reviewing the HD registry at the Neurogenetics Research Center-INCN from 2000 to 2014. Genotyping of HTT gene was confirmed using standard PCR and PAGE in accordance to protocols previously established. Results: Thirty-one late onset HD cases from 27 pedigrees were identified (9.42% of total HD cases, n = 329), 51.61% were male. Mean age at onset was 64.1 ± 4.2 and CAG repeats mean was 42.5 ± 2.5. We did not find significant correlation between age at onset and CAG repeats. 33.3% of cases were traced back to Cañete valley. Twenty-two cases had a positive family history, 14 of them with paternal transmission. Choreic movements and cognitive impairment were the main existing manifestations reported in this cohort, with lower frequency of psychiatric disturbances. Conclusions: This report of late onset HD affected individuals shows a mild phenotype expression of the disease, associated with low range of CAG repeats and up to 30% of cases with absence of clear family history. Cañete valley remains the region with more cases. [ABSTRACT FROM AUTHOR]

Published

2015

8. The distribution and risk effect of GBA variants in a large cohort of PD patients from Colombia and Peru.

Author

Velez-Pardo, Carlos, Lorenzo-Betancor, Oswaldo, Jimenez-Del-Rio, Marlene, Moreno, Sonia, Lopera, Francisco, Cornejo-Olivas, Mario, Torres, Luis, Inca-Martinez, Miguel, Mazzetti, Pilar, Cosentino, Carlos, Yearout, Dora, Waldherr, Sarah M., Zabetian, Cyrus P., and Mata, Ignacio F.

Subjects

*PARKINSON'S disease, *ETIOLOGY of Parkinson's disease, *PARKINSON'S disease & genetics, *DISEASE risk factors, *GENETIC mutation, *GLYCOSIDASES, *GAUCHER'S disease, *AGE of onset

Abstract

Background: Mutations in the glucocerebrosidase (GBA) gene are an important risk factor for Parkinson's disease (PD). However, most GBA genetic studies in PD have been performed in patients of European origin and very few data are available in other populations.Methods: We sequenced the entire GBA coding region in 602 PD patients and 319 controls from Colombia and Peru enrolled as part of the Latin American Research Consortium on the Genetics of Parkinson's disease (LARGE-PD).Results: We observed a significantly higher proportion of GBA mutation carriers in patients compared to healthy controls (5.5% vs 1.6%; OR = 4.3, p = 0.004). Interestingly, the frequency of mutations in Colombian patients (9.9%) was more than two-fold greater than in Peruvian patients (4.2%) and other European-derived populations reported in the literature (4-5%). This was primarily due to the presence of a population-specific mutation (p.K198E) found only in the Colombian cohort. We also observed that the age at onset was significantly earlier in GBA carriers when compared to non-carriers (47.1 ± 14.2 y vs. 55.9 ± 14.2 y; p = 0.0004).Conclusion: These findings suggest that GBA mutations are strongly associated with PD risk and earlier age at onset in Peru and Colombia. The high frequency of GBA carriers among Colombian PD patients (∼10%) makes this population especially well-suited for novel therapeutic approaches that target GBA-related PD. [ABSTRACT FROM AUTHOR]

Published

2019