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ABSTRACT The genus Bartonella encompasses 38 validated species of Gram-negative, facultative intracellular bacteria that colonize the endothelial cells and erythrocytes of a wide spectrum of mammals. To date, 12 Bartonella species have been recorded infecting humans, causing diseases of long historical characterization, such as cat scratch fever and trench fever, and emerging bartonellosis that mainly affect animal health professionals. For this reason, this study aimed to report a documented case of Bartonella bovis infecting a veterinarian from Mexico by the amplification, sequencing and phylogenetic reconstruction of the citrate synthase (gltA) and the RNA polymerase beta-subunit (rpoB) genes, and to report the natural course of this infection. To our knowledge, this work is the first to report the transmission of B. bovis via needlestick transmission to animal health workers in Latin America.
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ABSTRACT In this study, we report the presence of a female Amblyomma americanum tick attached to a former resident of the East Coast of the United States who moved to Mexico city. The amplification and sequencing of gene fragments of the 16S-rDNA and cytochrome c oxidase subunit 1 corroborated the identification of the species of the tick. Additionally, the presence of DNA of Rickettsia amblyommatis was confirmed. This work is the first report of an exotic tick of the genus Amblyomma in a traveler from the US to Mexico and represents the second record of an imported tick attached to humans in Mexico.
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Abstract Cutaneous leishmaniasis (CL) involves several differential diagnoses as it lacks a gold standard diagnostic test. Its diagnosis is easier in endemic regions; however, many cases come from travelers to endemic areas. A 22-year-old patient, who had recently visited Oaxaca, Mexico, developed two asymptomatic ulcers weeks later on the left auricle and the nose. Leishmania mexicana was identified using polymerase chain reaction. The patient was treated with imiquimod 5% cream three times/week, providing favorable results after 12 weeks, without relapse 2 months after therapy. To our knowledge, this is the first case of CL due to L. mexicana effectively treated with imiquimod.
Subject(s)
Humans , Young Adult , Leishmania mexicana , Leishmaniasis, Mucocutaneous , Leishmaniasis, Cutaneous/diagnosis , Leishmaniasis, Cutaneous/drug therapy , Imiquimod , MexicoABSTRACT
Abstract Murine typhus is a flea-borne disease caused by Rickettsia typhi, which was first detected in Mexico in 1927. It was not until 1996 that the first systematized study involving this pathogen was conducted in two coastal states of Mexico. We now report the first confirmed case of murine typhus in the state of Campeche, which occurred in a male patient who exhibited fever, thrombocytopenia, hyperbilirubinemia, and a rash. Furthermore, the patient reported having had previous contact with Rickettsia reservoirs.
Subject(s)
Humans , Male , Female , Adult , Typhus, Endemic Flea-Borne/diagnosis , Rickettsia typhi , Thrombocytopenia , Ceftriaxone/therapeutic use , Typhus, Endemic Flea-Borne/drug therapy , Typhus, Endemic Flea-Borne/blood , Polymerase Chain Reaction , Doxycycline/therapeutic use , Exanthema , Fever , MexicoABSTRACT
El dengue es una de las principales enfermedades transmitidas por vector. En la última década se convirtió en uno de los problemas de salud pública más importantes de México y América Latina. En el continente americano el dengue es considerado predominantemente un padecimiento de adultos, lo cual contrasta con los reportes de países asiáticos que consideran el dengue como una enfermedad principalmente pediátrica. Durante la última década se ha reportado el incremento de dengue juvenil y pediátrico en varios países de América. En la presente revisión, elaborada a partir de datos publicados por la Secretaría de Salud, se analiza la tendencia de aumento en la incidencia de dengue en la población juvenil e infantil de México durante los últimos 10 años.
Dengue is one of the principal vector-transmitted diseases leading to important public health problems in Mexico and Latin America. On the American continent this disease has been reported mostly in adults, which contrasts with Asian countries where pediatric dengue is more prominent. During the last decade a shift towards pediatric dengue has been reported in various countries of the American continent. This review, elaborated from data published by the Mexican Ministry of Health, focuses on dengue in Mexico during the last three decades, showing that during the last decade dengue fever and dengue hemorrhagic fever has begun to shift towards a juvenile and pediatric population.
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Background. In Mexico, a steady increase of patients with visceral leishmaniasis has been reported, especially in the states of Chiapas and Guerrero, yet only limited information exists on canine leishmaniasis in areas of visceral leishmaniasis in Mexico. A veterinary report of dogs with nonhealing cutaneous lesions in Pungarabato, Guerrero led us to investigate the possible presence of Leishmania infection in an area where Lutzomyia longipalpis and Lutzomyia evansi, both vectors of Leishmania infantum, have been described. Methods. We analyzed skin lesions of 25 dogs by immunohistochemistry and PCR. Results. We found a 60% prevalence of Leishmania-infected dogs, the infection rate being higher in males than females. Thus, we established a new focus of canine leishmaniasis, and although to date no patients have been reported in this municipality, it is close to and shares the same ecological characteristics of dry tropical forests as regions where visceral leishmaniasis has been reported in Mexico. We also include updated information of localities of visceral leishmaniasis in Mexico as well as the distribution of possible sand fly vectors. Conclusions. Our data show the need to ascertain the magnitude of this new focus in view of the current data on human visceral leishmaniasis, a disease that is surging in Mexico.
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Antecedentes: Los macrófagos son células de la respuesta inmune que reconocen patrones moleculares asociados a patógenos (PAMP) mediante receptores presentes en la superficie de la célula como en compartimentos intracelulares, como los TLR (toll like receptors). Distintos TLR reconocen ligandos que comparten múltiples patógenos. La unión de TLR con su ligando desencadena una cascada de señalización que termina en la producción de citocinas y moléculas coestimuladoras a través de la translocación de NF-κB al núcleo. Nuestro grupo demostró que el lipofosfoglucano de Leishmania es un ligando de TLR2 que activa células NK. Schieicher y cols.12 informo recientemente la activación de células dendríticas plasmacitoides con ADN genómico de Leishmania infantum a través de TLR9, con alta producción de IFN tipo I. Objetivo: En el presente trabajo exploramos si el ADN de Leishmania mexicana contiene motivos CpG no metilados capaces de activar al macrófago murino derivado de médula ósea, como ha sido descrito anteriormente para motivos CpG no metilados de ADN bacteriano. Resultados y conclusiones: Encontramos que el ADN de Leishmania mexicana posee motivos CpG no metilados que activan macrófagos murinos de la cepa BALB/c, llevando a la producción de citocinas proinflamatorias como TNFα e IL12P40 y a la sobreexpresión del mARN de TLR9.
BACKGROUND: Macrophages are immune system cells that recognize pathogen associated molecular patterns (PAMPs) through receptors that can be located on the cell membrane or in intracellular compartments, such as the TLR (toll like receptors). Different TLRs bind to ligands shared among multiple pathogens. The binding of ligands to TLRs induces a signaling cascade that leads to cytokine and co-stimulatory molecule production due to the nuclear translocation of NF-kappaB. We demonstrated that Leishmania lipophosphoglycan (LPG) is a ligand for TLR2, leading to NK-cell activation. Schieicher et al. recently reported that genomic DNA from Leishmania infantum activates plasmacitoid dendritic cells through TLR9, leading to IFN type I production. OBJECTIVE: In the present study we explored wether Leishmania mexicana DNA contained non-methylated CpG motifs able to activate murine bone marrow derived macrophages, as previously described for bacterial DNA containing CpG motifs. RESULTS AND CONCLUSIONS: We observed that Leishmania mexicana DNA contains non-methylated CpG morifs able ofactivating murine bone marrow derived macrophages, leading to the production of proinflammatory cytokines such as TNFalpha and IL- 12(P40) as well as the over expression of mRNA for TLR9.
Subject(s)
Animals , Mice , DNA, Protozoan/physiology , Leishmania mexicana/genetics , Macrophages/metabolism , Toll-Like Receptor 9/biosynthesis , Mice, Inbred BALB CABSTRACT
OBJETIVO: Examinar la bibliografía relacionada con la participación de los linfocitos T CD8+ en la reacción inmunitaria a especies de Leishmania causantes de leishmaniasis cutánea. En esta enfermedad se ha resaltado la intervención de macrófagos, células dendríticas, NK y células T CD4+; sin embargo, es poco lo que se conoce de las células T CD8+. Los trabajos en modelos murinos señalan que la participación de las células CD8+ sucede a través de la producción de IFN-gamma, aunque su capacidad citotóxica puede desempeñar una función importante, como lo demuestran los hallazgos en seres humanos. La forma como se activan las células citotóxicas CD8+ es un enigma. Es posible que las células dendríticas realicen esa labor a través de mecanismos que incluyen transpresentación de antígenos. Comprender la contribución de este subtipo celular en la respuesta inmunitaria a Leishmania aportará novedosos conocimientos sobre la fisiopatogenia de la leishmaniasis, lo cual hará posible desarrollar nuevos enfoques terapéuticos para esta parasitosis.
OBJECTIVE: Review of the literature on the role of CD8+ T cell in the immune response against Leishmania species that cause cutaneous leishmaniasis. The role of macrophages, dendritic cells, CD4 T cells and NK cells has been extensively analyzed in leishmaniasis, yet very little knowledge has been gained on CD8+ T cells in this disease. Murine models of leishmaniasis suggest that CD8+ T cells participate through IFNg production, yet their cytotoxic capacity may also play a crucial role, as has been found in human disease. It is an enigma what mechanisms underlie the CD8+ T cell activation. It is possible that dendritic cells activate CD8+ T cells through mechanisms that include antigen traspresentation. A better understanding of CD8+ T cells in the immune response against Leishmania will undoubtedly provide new insights into the physiopathogenesis of the disease that could lead to new therapeutic approaches against leishmaniasis.
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Humans , Leishmaniasis, Cutaneous/immunology , T-Lymphocytes, Cytotoxic/immunologyABSTRACT
Las formas más frecuentes de leishmaniosis en México son la leishmaniosis cutánea localizada (LCL), un padecimiento relativamente benigno, y la leishmaniosis cutánea diseminada (LCD), de evolución generalmente mortal. La caracterización fenotípica de parásitos aislados de pacientes con LCL y LCD ha revelado, que el agente casual de ambos cuadros clínicos de Leishmania mexicana mexicana. Sin embargo la resistencia a medicamentos y la virulencia inesperada en algunos pacientes hacen sospechar una posible introducción de nuevas especies en México o bien mutaciones intraespecie. En este trabajo realizamos un análisis genotípico del kADN de leishmanias aisladas de pacientes con LCL y LCD, mediante endonucleasas de restricción (Hae II.I y Hpa II) y RAPD (amplificacion aleatoria de ADN polimórfico con oligonucleótidos no específicos). Encontramos polimorfismo en las digestiones sugestivas de la introducción de nuevas especies en México, lo cual se tendrá que confirmar con PCR especie-especificos. Mediante el RAPD detectamos una ligera diferencia entre un paciente con LCD y otros con LCL. Esta variación intraespecie pudiera ser una de las posibles causas de diseminación del parásito.