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Leptospirosis is a disease caused by the bacteria of the Leptospira genus, which can usually be acquired by humans through contact with urine from infected animals; it is also possible for this urine to contaminate soils and bodies of water. The disease can have deadly consequences in some extreme cases. Fortunately, until now, patients with leptospirosis have responded adequately to treatment with doxycycline and azithromycin, and no cases of antibiotic resistance have been reported. However, with the extensive use of such medications, more bacteria, such as Staphylococci and Enterococci, are becoming resistant. The purpose of this study is to determine the presence of genes related to antibiotic resistance in the Leptospira genus using bioinformatic tools, which have not been undertaken in the past. Whole genomes from the 69 described Leptospira species were downloaded from NCBI's GeneBank and analyzed using CARD (The Comprehensive Antibiotic Resistant Database) and RAST (Rapid Annotations using Subsystem Technology). After a detailed genomic search, 12 genes associated with four mechanisms were found: resistance to beta-lactamases, vancomycin, aminoglycoside adenylyltransferases, as well as multiple drug efflux pumps. Some of these genes are highly polymorphic among different species, and some of them are present in multiple copies in the same species. In conclusion, this study provides evidence of the presence of genes related to antibiotic resistance in the genomes of some species of the genus Leptospira, and it is the starting point for future experimental evaluation to determine whether these genes are transcriptionally active in some species and serovars.
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Resumen Introducción: existen varios Receptores Tirosina Quinasa que están involucrados en el desarrollo, crecimiento y progresión de las células tumorales, por ejemplo, en los glioblastomas se ha encontrado que por un posible desequilibrio de ligamiento los genes PDGFRA, KIT y KDR, ubicados en el brazo largo del cromosoma 4 (4q11-q12), podrían estar relacionados con la progresión de esta neoplasia. Objetivo: reportar dos casos clínicos de pacientes con diagnóstico de glioblastoma y mutaciones en los genes PDGFRA, KIT, KDR, y su relación con un peor desenlace. Casos clínicos: en este artículo se presenta el caso de dos pacientes con glioblastomas que presentan mutaciones en los genes anteriormente mencionados resultado de la secuenciación de un panel genético que evalúa 324 genes y 37 fusiones génicas y la progresión clínica acelerada durante el transcurso de la enfermedad. Conclusión: los cambios producidos en los glioblastomas por las mutaciones en los receptores tirosina quinasa a nivel biológico podrían describir una mayor capacidad proliferativa del tumor, lo que en el ámbito clínico se ha evidenciado como un peor pronóstico para el paciente, de ahí nace la necesidad de tener paneles genéticos que ayuden a identificar el perfil tumoral, e incentivar más estudios clínicos relacionados a fármacos que tengan como objetivo dichos receptores.
Abstract Introduction: there are several Tyrosine Kinase Receptors that are involved in the development, growth and progression of tumor cells, for example, in glioblastomas it has been found that due to a possible linkage imbalance the PDGFRA, KIT and KDR genes, located in the arm length of chromosome 4 (4q11-q12), which could be related to the progression of this neoplasm. Objective: to report two clinical cases of patients diagnosed with glioblastoma and mutations in the PDGFRA, KIT, and KDR genes, and their relationship with a worse outcome. Clinical cases: this article presents the case of two patients with mutations in the genes, the result of a genetic panel that evaluated 324 genes and 37 gene fusions and accelerated clinical progression during the course of the disease. Conclusion: the changes produced in glioblastomas by mutations in receptor tyrosine kinases at the biological level describe a greater proliferative capacity of the tumor, which in the clinical setting has been evidenced as a worse prognosis for the patient, hence the need for have genetic panels that help identify the tumor profile and encourage more clinical studies related to drugs that target those receptors.
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Introduction: Amyotrophic lateral sclerosis is a neurodegenerative disease with a possible multifactorial origin characterized by the progressive degeneration of motor neurons. There is a relatively high prevalence of this disease in Antioquia; however, there is no published genetic study to date in Colombia. Despite its unknown etiopathogenesis, more genetic risk factors possibly involved in the development of this disease are constantly found. Objetives: To evaluate G93A and D90A mutations in SOD1 gene and a short tandem repeat in C9orf72 within a cohort of amyotrophic lateral sclerosis patients from Antioquia, Colombia. Materials y methods: Thirty-four patients previously diagnosed with amyotrophic lateral sclerosis were included in the study. Peripheral blood samples were used for DNA extraction and genotyping. Results: No mutations were found in SOD1 (G93A and D90A) in any of the patients, while C9orf72 exhibited an allele with a statistically significant high prevalence in the study sample (8 hexanucleotide repeats of CAGCAG). Conclusions: These results suggest an association between this short tandem repeat (STR) in C9orf72 and the presence of amyotrophic lateral sclerosis in the studied population. However, this association should be established in a larger sample size and with controls from the same population. In addition, there also seems to be a genetic anticipation effect for the disease regarding this locus, since patients with this genotype present an earlier onset.
Introducción. La esclerosis lateral amiotrófica es una enfermedad neurodegenerativa con un posible origen multifactorial, caracterizado por una degeneración progresiva de las neuronas motoras. Hay una gran prevalencia relativa de esta enfermedad en Antioquia; sin embargo, no hay publicaciones de estudios genéticos en Colombia. A pesar de su etiopatogénesis desconocida, hay varios factores de riesgo genético que se encuentran constantemente en el desarrollo de esta enfermedad. Objetivo. Evaluar las mutaciones G93A y D90A del gen SOD1 y una repetición corta en tándem (Short Tandem Repeat, STR) en el locus C9orf72, en una cohorte de pacientes con esclerosis lateral amiotrófica en Antioquia, Colombia. Materiales y métodos. Se incluyeron 34 pacientes previamente diagnosticados en el estudio. Una muestra de sangre periférica se usó para extraer el ADN y, posteriormente, genotipificarlo. Resultados. No se encontraron mutaciones en el gen SOD1 (G93A y D90A), mientras que el C9orf72 exhibe un alelo con una significativa prevalencia en los pacientes del estudio (8 repeticiones del hexanucleótido G4C2). Conclusiones. Se sugiere una asociación entre la repetición en tándem en C9orf72 y la presencia de la esclerosis lateral amiotrófica en la población estudiada. Sin embargo, se sugiere hacer estudios adicionales e incluir un grupo control de la misma población. Además, se detecta un fenómeno de anticipación genética de la enfermedad, dado que los pacientes con el alelo de 8 repeticiones en C9orf72 presentan una edad temprana de aparición de los síntomas.
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Esclerosis Amiotrófica Lateral/genética , Mutación , Enfermedades Neurodegenerativas , GenesRESUMEN
Resumen El cáncer de mama invasor es una neoplasia de origen multifactorial en el cual están involucrados tanto componentes genéticos, como no genéticos, los cuales pueden modular su aparición temprana. El objetivo de este estudio es evaluar la participación de los componentes genéticos. Metodología: se analizaron 165 mujeres con cáncer de mama pertenecientes a la población "paisa" y estratificadas por edad de diagnóstico. Se evaluaron variables no genéticas y, de forma indirecta, variables genéticas usando marcadores tipo short tándem repeats (STR). Resultados: no se detectaron diferencias en cuanto a los factores de riesgo no genético entre pacientes mayores y menores de 50 años, ni al evaluar los genes de forma individual. Al comparar combinaciones genéticas se detectaron dos interacciones génicas en mujeres menores de 50 años: BRCA2-BRCA1 (p= 0,04) y BRCA2-ATM (p= 0,008). Conclusión: estos resultados sugieren la participación de la interacción de dichos genes en la aparición de cáncer de mama antes de los 50 años. Dado que el estudio se hizo con marcadores indirectos es necesario realizar estudios posteriores para identificar las mutaciones funcionales que soporten estos hallazgos.
Abstract Invasive breast cancer is a multifactorial neoplasm, involving both genetic and non-genetic components that modulate their early appearance of the disease. The aim of this study was to evaluate the contribution of genetic factors and disease. Methodology: 165 breast cancer patients stratified by age and belonging to the "paisa" population participated in the study. No genetic variables were controlled, and genetic variables were indirectly evaluated using short tandem repeats (STR) markers. Results: No differences were detected in non-genetic risk factors among patients older and younger than 50 years, not even in the individual evaluation of genes. When genetic combinations were evaluated, two interactions were detected in women younger than 50 years: BRCA2-BRCA1 (p= 0,04) and BRCA2-ATM (p= 0,008). Conclusion: These results suggest the involvement of gene interaction BRCA1-BRCA2 and BRCA2-ATM genes in the case of early onset of breast cancer (before the age of 50). Since the study was made with indirect markers, is necessary to perform further studies to identify the functional mutations that support these findings.