Your search keyword '"Kim, Chong Ae"' showing total 13 results

1. New insights in mucopolysaccharidosis type VI: Neurological perspective

Author

Borlot, Felippe, Arantes, Paula Ricci, Quaio, Caio Robledo, da Silva Franco, José Francisco, Lourenço, Charles Marques, Bertola, Debora Romeo, and Kim, Chong Ae

Published

2014

2. LDL receptor-related protein 5 (LRP5) affects bone accrual and eye development

Author

Gong, Yaoquin, Slee, Roger B., Fukai, Naomi, Rawadi, Georges, Roman-Roman, Sergio, Reginato, Anthony M., Wang, Hongwei, Cundy, Tim, Glorieux, Frencis H., Lev, Dorit, Zucharin, Margaret, Oexle, Konrad, Marcelino, Jose, Suwairi, Wafaa, Heeger, Shauna, Sabatakos, George, Apte, Suneel, Adkins, William N., Allgrove, Aeslan-Kirshner, Mine, Batch, Jennifer A., Beighton, Peter, Black, Graeme C. M., Boles, Richard G., Boon, Laurence M., Borone, Carla, Brunner, Han G., Carle, Georgas F., Dallapiccola, Bruno, Paepe, Anne de, Floege, Barbara, Halfhide, Melissa Lees, Hall, Bryan, Hennekam, Raoul C., Hirose, Tatsou, Jans, Ab, Juppner, Harald, Kim, Chong Ae, Keppler-Noreuil, Kim, Kohlschuetter, Alfried, LaCombe, Didier, Lambert, MArie, Lemyre, Emmanuelle, Letteboer, Tom, Peltonen, Leena, Ramesar, Rajkumar S., Romanengo, Marta, Somer, Hannu, Steichen-Gersdorf, Elisabeth, Steinman, beat, Sullivan, Beth, Superti-Firga, Andrea, Swoboda, Walter, Boogaard, MArie-Jose van der, Hul, Wim van, Vikkula, Miika, Votruba, Marcela, Zabel, Bernhard, Garcia, Teresa, Baron, Roland, Olsen, Bjorn R., and Warman, Matthew L.

Subjects

Cell research -- Analysis, Proteins -- Physiological aspects, Lipoproteins -- Physiological aspects, Bones -- Growth, Biological sciences

Abstract

Research has been conducted on the low peak mass that presents significant risk factor for osteoporosis. The effect of the LRP5 encoding the low-density lipoprotein receptor-related protein 5 on the bone mass accrual during growth has been investigated and the results are reported.

Published

2001

3. Congenital abnormalities in Brazilian children associated with misoprostol misuse in first trimester of pregnancy

Author

Gonzalez, Claudette Hajaj, Marques-Dias, Maria Joaquina, Kim, Chong Ae, Sugayama, Sofia M.M., Da Paz, Jose Albino, Huson, Susan M., and Holmes, Lewis B.

Subjects

Cytotec (Medication) -- Adverse and side effects, Misoprostol -- Adverse and side effects, Clubfoot -- Causes of, Arthrogryposis -- Causes of, Birth defects -- Causes of, Abortifacients -- Adverse and side effects

Published

1998

4. Genetic Disorders in Prenatal Onset Syndromic Short Stature Identified by Exome Sequencing.

Author

Homma, Thais Kataoka, Freire, Bruna Lucheze, Honjo Kawahira, Rachel Sayuri, Dauber, Andrew, Funari, Mariana Ferreira de Assis, Lerario, Antônio Marcondes, Nishi, Mirian Yumie, Albuquerque, Edoarda Vasco de, Vasques, Gabriela de Andrade, Collett-Solberg, Paulo Ferrez, Miura Sugayama, Sofia Mizuho, Bertola, Debora Romeo, Kim, Chong Ae, Arnhold, Ivo Jorge Prado, Malaquias, Alexsandra Christianne, and Jorge, Alexander Augusto de Lima

Abstract

Objective: To perform a prospective genetic investigation using whole exome sequencing of a group of patients with syndromic short stature born small for gestational age of unknown cause.Study Design: For whole exome sequencing analysis, we selected 44 children born small for gestational age with persistent short stature, and additional features, such as dysmorphic face, major malformation, developmental delay, and/or intellectual disability. Seven patients had negative candidate gene testing based on clinical suspicion and 37 patients had syndromic conditions of unknown etiology.Results: Of the 44 patients, 15 (34%) had pathogenic/likely pathogenic variants in genes already associated with growth disturbance: COL2A1 (n = 2), SRCAP (n = 2), AFF4, ACTG1, ANKRD11, BCL11B, BRCA1, CDKN1C, GINS1, INPP5K, KIF11, KMT2A, and POC1A (n = 1 each). Most of the genes found to be deleterious participate in fundamental cellular processes, such as cell replication and DNA repair.Conclusions: The rarity and heterogeneity of syndromic short stature make the clinical diagnosis difficult. Whole exome sequencing allows the diagnosis of previously undiagnosed patients with syndromic short stature. [ABSTRACT FROM AUTHOR]

Published

2019

5. Expanding the Phenotype of 8p23.1 Deletion Syndrome: Eight New Cases Resembling the Clinical Spectrum of 22q11.2 Microdeletion.

Author

Montenegro, Marília Moreira, Camilotti, Débora, Quaio, Caio Robledo D'Anglioli Costa, Gasparini, Yanca, Zanardo, Évelin Aline, Rangel-Santos, Andreia, Novo-Filho, Gil Monteiro, Francisco, Gleyson, Liro, Lucas, Nascimento, Amom, Chehimi, Samar Nasser, Soares, Diogo Cordeiro Queiroz, Krepischi, Ana C.V., Grassi, Marcília Sierro, Honjo, Rachel Sayuri, Palmeira, Patricia, Kim, Chong Ae, Carneiro-Sampaio, Magda Maria Sales, Rosenberg, Carla, and Kulikowski, Leslie Domenici

Published

2023

6. The first Brazilian clinical report of Kleefstra syndrome, including semicircular canals agenesis as a possible phenotype expansion.

Author

Da Cás, Eduardo, Pires, Lucas V.L., Linnenkamp, Bianca D.W., Allegro, Marcella C., Honjo, Rachel S., Bertola, Débora R., Aoi, Hiromi, Matsumoto, Naomichi, and Kim, Chong Ae

Subjects

*SEMICIRCULAR canals, *CONGENITAL heart disease, *BRAZILIANS, *HUMAN abnormalities, *HEARING disorders, *AGENESIS of corpus callosum

Abstract

to report the first case series of Brazilian children diagnosed with Kleefstra syndrome, present a possible phenotype expansion to the syndrome and to raise physicians' awareness for this rare disease. seven patients with confirmed KS were evaluated, including 5 males and 2 females. Abnormal prenatal findings were observed in 4 patients. Most patients were born at term, with normal birth measurements. All patients had neurodevelopmental delay and 6 evolved with intellectual disability. Hearing loss was present in 57.1% of patients and 28.7% had congenital heart disease. In males, cryptorchidism was present in 75%. Despite the facial dysmorphisms, only 2 out of 7 patients had a pre-test clinical suspicion of KS. One specific patient presented bilateral agenesis of the semicircular canals, a very rare ear manifestation in Kleefstra syndrome, representing a possible phenotype expansion of the syndrome. this report aims to promote awareness among physicians evaluating patients in a context of neurodevelopmental delay or congenital malformations, especially congenital heart defects. We also highlight a possible phenotype expansion of the syndrome, with a case of semicircular anomaly, not reported in this syndrome so far. [ABSTRACT FROM AUTHOR]

Published

2024

7. Auditory hypersensitivity in Williams syndrome.

Author

Silva, Liliane Aparecida Fagundes, Kawahira, Rachel Sayuri Honjo, Kim, Chong Ae, and Matas, Carla Gentile

Subjects

*WILLIAMS syndrome, *ACOUSTIC reflex, *HYPERACUSIS, *AUDITORY neuropathy, *INDIVIDUAL development, *HEARING disorders, *LOUDNESS

Abstract

The objective of this study was to investigate auditory hypersensitivity in WS and to evaluate hyperacusis through standardized protocols, checking if it can be associated with the absence of acoustic reflexes in people with WS. The study was performed in 17 individuals with WS, aged between seven and 17 years old (10 males and seven females), and 17 individuals with typical development age- and gender-matched to individuals with WS. Statistical tests were used to analyze the responses collected with the Loudness Discomfort Level (LDL) test as well as ipsilateral and contralateral reflex responses. Auditory hypersensitivity was commonly found. Individuals with WS had phonophobia and were less tolerant to high sound intensity, presenting a reduced discomfort threshold compared to those with typical development. However, hyperacusis was found in 35.29% of individuals with WS and was mild in 50% of cases. There was an association between hyperacusis and acoustic reflex responses, and individuals with absence of the contralateral acoustic reflex were more likely to have hyperacusis. Individuals with WS have a high prevalence of auditory hypersensitivity, with the presence of phonophobia; however, hyperacusis was not as prevalent and may be associated with the absence of contralateral acoustic reflexes. [ABSTRACT FROM AUTHOR]

Published

2021

8. Abnormal auditory event-related potentials in Williams syndrome.

Author

Fagundes Silva, Liliane Aparecida, Honjo Kawahira, Rachel Sayuri, Kim, Chong Ae, and Matas, Carla Gentile

Subjects

*WILLIAMS syndrome, *EVOKED potentials (Electrophysiology), *INTERSTIMULUS interval, *HEARING disorders, *MUSIC appreciation, *MIDDLE ear, *OTOACOUSTIC emissions

Abstract

Individuals with Williams Syndrome (WS) have specific auditory characteristics, including hypoacusis and hyperacusis, and music appreciation skills. Little is known about the functionality of the central auditory nervous system (CANS) for sound processing in WS. Thus, the objective of the present study was to evaluate the functionality of the CANS in individuals with WS, based on auditory event-related potentials, as far as cognitive and behavioral aspects are concerned. The study was carried out with 17 individuals, seven females and ten males, between seven and 17 years old, with WS, and 17 individuals with typical development matched by sex and chronological age to individuals with WS. None of these individuals had middle ear impairment or hearing loss. The subjects were evaluated for intelligence quotient, loudness discomfort level, and auditory event-related potentials with Tone Burst stimuli, on the oddball paradigm; the parents also answered the MTA-SNAP-IV questionnaire. Hyperacusis was found in six WS individuals and two individuals with typical development. In the present study, WS individuals present longer latency and reduced amplitude for P1, N1, N2 and P3 components. These results, suggesting a delay and hypoactive responses of the CANS in this syndrome, that cannot be related to the cognitive or behavioral aspects of these individuals, but it indicates a cortical immaturity to process acoustic stimuli. [ABSTRACT FROM AUTHOR]

Published

2021

9. Study of the peripheral and central auditory pathways in patients with mucopolysaccharidosis.

Author

Chimelo, Flávia Teixeira, Silva, Liliane Aparecida Fagundes, Neves-Lobo, Ivone Ferreira, Kim, Chong Ae, and Matas, Carla Gentile

Subjects

*HEARING disorder diagnosis, *AUDITORY evoked response, *NEURAL pathways, *AUDITORY perception, *ACOUSTIC reflex, *OTOSCOPY, *SENSORINEURAL hearing loss, *COMPARATIVE studies, *AUDIOMETRY, *DESCRIPTIVE statistics, *MUCOPOLYSACCHARIDOSIS, *BRAIN stem

Abstract

• Mucopolysaccharidosis is a group of progressive hereditary diseases. • Individuals with mucopolysaccharidosis are risk of auditory pathway impairment. • Audiological assessments of peripheral and central auditory pathways. • Sensorineural hearing loss in Individuals with mucopolysaccharidosis. To investigate the peripheral and central auditory pathways in mucopolysaccharidosis (MPS) individuals. The research sample comprised 15 individuals (one female and 14 males), aged 8 to 46 years. The following procedures were used: medical history survey, otoscopy, speech and pure-tone threshold audiometry, acoustic immittance measures, and central auditory pathway assessment with brainstem auditory evoked potentials (BAEP) and long-latency auditory evoked potentials (LLAEP). The pure-tone audiometry identified hearing loss in 13 individuals, and more than 90 % of the hearing loss was sensorineural. The degree of hearing loss was between mild to moderately severe with descendent configuration. Type A tympanogram predominated, and acoustic reflexes were present according to the types and degrees of hearing loss. Among the individuals with abnormal BAEP, longer wave III and V absolute latencies were the main findings. In addition, the unilateral absence of wave I was observed in two cases. In the LLAEP, longer latencies were observed in 14 individuals, and the most impaired components were the P1 and P3 in children and adolescents and the P2, N2 and P3 in adult individuals. The peripheral auditory pathway assessment revealed a predominantly sensorineural hearing loss, affecting mainly high frequencies, and in the central pathway was observed abnormal brainstem and cortical auditory processing in individuals with MPS. [ABSTRACT FROM AUTHOR]

Published

2024

10. CD4+CD25highFoxp3+ Treg deficiency in a Brazilian patient with Gaucher disease and lupus nephritis.

Author

Matta, Marina Cadena, Soares, Diogo Cordeiro, Kerstenetzky, Marcelo Soares, Freitas, Augustus Cesar Pinto, Kim, Chong Ae, and Torres, Leuridan Cavalcante

Subjects

*GAUCHER'S disease, *LUPUS nephritis, *CD4 antigen, *CD5 antigen, *FORKHEAD transcription factors, *PROTEIN deficiency, *BRAZILIANS, *DISEASES

Abstract

Gaucher Disease (GD) is a rare autosomal recessive disorder caused by the deficient activity of beta-glucocerebrosidase. GD is one of the lysosomal storage diseases with the most remarkable alterations in the immune system, and that may manifest clinically as autoimmune disorders and malignancy. We reported the immunological evaluation of a patient with GD and lupus nephritis. Decreased absolute values of T, and NK, and an inversion of CD4 + /CD8 + ratio, low levels of IgM and normal B cells were found when compared to reference values in a Brazilian population. Absence ofCD4 + CD25 high Foxp3 + Treg and high levels of total NKT, iNKT cells and CD8 + iNKT subsets were also observed when compared to the healthy control and GD patient without lupus nephritis. Treg subset and CD8 + iNKT abnormalities might be involved in severe lupus nephritis in a GD patient. We conclude by emphasizing the importance of the immunological evaluation on early diagnosis of autoimmunity contributing to reduce mortality and morbidity of these patients. [ABSTRACT FROM AUTHOR]

Published

2016

11. A study of EEG and epilepsy profile in Wolf–Hirschhorn syndrome and considerations regarding its correlation with other chromosomal disorders

Author

Valente, Kette D., Freitas, Alessandra, Fiore, Lia A., and Kim, Chong Ae

Subjects

*EPILEPSY, *ELECTROENCEPHALOGRAPHY

Abstract

Wolf–Hirschhorn syndrome (WHS) is a genetic disorder caused by a deletion of the short arm of chromosome 4. Sgro` et al. described an electroclinical profile for WHS, but data regarding this issue are scarce. We report an 8-year-old girl presenting the classic phenotype for WHS, confirmed by FISH test. Epilepsy started during infancy with myoclonic seizures. Later, she presented atypical absences, which gradually increased in frequency, and at the age of 2.5 years, she presented a non-convulsive status epilepticus. Epilepsy was controlled with valproate at the age of 6 years. Serial EEGs were performed and showed unusual bursts of generalized, high amplitude delta waves with superimposed low–moderate amplitude sharp waves. A literature review was performed and our case was compared to others, where EEG and/or epilepsy were addressed. Our case and previously published data show that WHS presents a stereotyped epilepsy profile and EEG patterns. A discussion concerning similarities between these findings and those observed in Angelman syndrome has been performed, since in both syndromes, GABA genes are involved and may play a role in the pathogenesis. Although fascinating, this theory is simplistic, since patients with Angelman syndrome without GABA deletion may present epilepsy and EEG abnormalities. Another issue is the striking overlap regarding these features, between WHS and Pitt–Rogers–Danks syndrome, which may be a key in showing that these disorders could be a spectral variation of the same entity. [Copyright &y& Elsevier]

Published

2003

12. The first cardiac transplant experience in a patient with mucopolysaccharidosis

Author

Grinberg, Henrique, Quaio, Caio Robledo D'Angioli Costa, Avila, Monica Samuel, Ferreira, Silvia Moreira Ayub, Vieira, Marcelo Luiz Campos, Benvenuti, Luiz Alberto, Kim, Chong Ae, and Bocchi, Edimar Alcides

Subjects

*HEART transplant recipients, *MUCOPOLYSACCHARIDOSIS, *HEART biopsy, *CARDIAC hypertrophy, *HEART cells, *HEART failure, *GLYCOSAMINOGLYCANS

Abstract

Abstract: Hunter syndrome (MPSII) is a rare X-linked lysosomal storage disorder that can affect multiple systems but primarily affects the heart. We report the case of a previously asymptomatic 23-year-old patient who had an attenuated form of MPSII and presented with refractory heart failure that required a heart transplant. The diagnosis was confirmed by detection of an increase in urinary excretion of glycosaminoglycans, a deficiency in enzymatic activity, and molecular analysis. A myocardial biopsy revealed hypertrophic cardiomyocytes, mild fibrosis, and lysosomal storage in interstitial cells. Molecular analysis identified a novel mutation in the iduronate-2-sulfatase gene. Although the clinical outcome was not favorable, we believe that this approach may be valid in end-stage heart failure. [Copyright &y& Elsevier]

Published

2012

13. Using a combination of MLPA kits to detect chromosomal imbalances in patients with multiple congenital anomalies and mental retardation is a valuable choice for developing countries

Author

Jehee, Fernanda Sarquis, Takamori, Jean Tetsuo, Vasconcelos Medeiros, Paula F., Pordeus, Ana Carolina B., Latini, Flavia Roche M., Bertola, Débora Romeo, Kim, Chong Ae, and Passos-Bueno, Maria Rita

Subjects

*GENE amplification, *CHROMOSOME abnormalities, *KARYOTYPES, *HUMAN abnormalities, *INTELLECTUAL disabilities, *WILLIAMS syndrome, *GENETIC testing, DEVELOPING countries

Abstract

Abstract: Conventional karyotyping detects anomalies in 3–15% of patients with multiple congenital anomalies and mental retardation (MCA/MR). Whole-genome array screening (WGAS) has been consistently suggested as the first choice diagnostic test for this group of patients, but it is very costly for large-scale use in developing countries. We evaluated the use of a combination of Multiplex Ligation-dependent Probe Amplification (MLPA) kits to increase the detection rate of chromosomal abnormalities in MCA/MR patients. We screened 261 MCA/MR patients with two subtelomeric and one microdeletion kits. This would theoretically detect up to 70% of all submicroscopic abnormalities. Additionally we scored the de Vries score for 209 patients in an effort to find a suitable cut-off for MLPA screening. Our results reveal that chromosomal abnormalities were present in 87 (33.3%) patients, but only 57 (21.8%) were considered causative. Karyotyping detected 15 abnormalities (6.9%), while MLPA identified 54 (20.7%). Our combined MLPA screening raised the total detection number of pathogenic imbalances more than three times when compared to conventional karyotyping. We also show that using the de Vries score as a cut-off for this screening would only be suitable under financial restrictions. A decision analytic model was constructed with three possible strategies: karyotype, karyotype + MLPA and karyotype + WGAS. Karyotype + MLPA strategy detected anomalies in 19.8% of cases which account for 76.45% of the expected yield for karyotype + WGAS. Incremental Cost Effectiveness Ratio (ICER) of MLPA is three times lower than that of WGAS, which means that, for the same costs, we have three additional diagnoses with MLPA but only one with WGAS. We list all causative alterations found, including rare findings, such as reciprocal duplications of regions deleted in Sotos and Williams–Beuren syndromes. We also describe imbalances that were considered polymorphisms or rare variants, such as the new SNP that confounded the analysis of the 22q13.3 deletion syndrome. [Copyright &y& Elsevier]

Published

2011