Your search keyword '"Duque, Thabata"' showing total 4 results

1. Leishmania (V.) braziliensis infection promotes macrophage autophagy by a LC3B-dependent and BECLIN1-independent mechanism.

Author

Duque, Thabata Lopes Alberto, Serrão, Thamires Christinne de Souza Lopes Cruz, Gonçalves, Antônio José da Silva, Pinto, Eduardo Fonseca, Oliveira-Neto, Manoel Paes, Pirmez, Claude, Pereira, Luiza de Oliveira Ramos, and Menna-Barreto, Rubem Figueiredo Sadok

Subjects

*AUTOPHAGY, *MACROPHAGES, *LEISHMANIA, *INFECTION, *PARACOCCIDIOIDOMYCOSIS

Abstract

• In early infection, THP-1 macrophages cultured with Leishmania braziliensis delayed LC3 mobilization. • During late infection, the percentage of LC3+ cells increased in infected culture. • Autophagy induction, through rapamycin treatment or starvation, reduced infection at 24h. • Autophagy downregulation by LC3B but not BECLIN1 siRNA increased infection. Leishmania (Viannia) braziliensis is one of the main etiological agents of tegumentary leishmaniasis in Latin America. The establishment of a successful infection in host cells requires several key events including phagocytosis, phagolysosomal maturation impairment, and parasite replication. Autophagy is accountable for the physiological turnover of cellular organelles, degradation of macromolecular structures, and pathogen elimination. In many cases, autophagy control leads to a successful infection, both impairing pathogen elimination or providing nutrients. Here, we have investigated the relationship between autophagy and L. braziliensis infection. We observed that BECLIN1 expression was upregulated early on infection in both in vitro macrophage cultures and biopsies of cutaneous lesions from L. braziliensis infected patients. On the other hand, LC3B expression was downregulated in cutaneous lesions biopsies. A transient pattern of LC3+ cells was observed along L. braziliensis infection, but the number of LC3 puncta did not vary. Additionally, autophagy induction, with rapamycin treatment or through starvation, reduced infection. As expected, rapamycin increased the percentage of LC3+ cells and the number of puncta, but the presence of parasite restricted this effect, indicating LC3-associated autophagy impairment by L. braziliensis. Finally, silencing LC3B but not BECLIN1 promoted infection, confirming BECLIN1 independent and LC3B -related control by the parasite. Taken together, these data indicate macrophage autophagic machinery manipulation by L. braziliensis , resulting in successful establishment and survival into the host cell. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2021

2. The induction of host cell autophagy triggers defense mechanisms against Trypanosoma cruzi infection in vitro.

Author

Duque, Thabata L.A., Siqueira, Mariana S., Travassos, Leonardo H., Moreira, Otacílio C., Bozza, Patrícia T., Melo, Rossana C.N., Henriques-Pons, Andrea, and Menna-Barreto, Rubem F.S.

Subjects

*TRYPANOSOMA cruzi, *PARASITE life cycles, *HEART cells, *AUTOPHAGY, *PERITONEAL macrophages, *CELL death, *CELL anatomy, *LIFE cycles (Biology)

Abstract

• Parasites increase LC3 in cardiac cells and peritoneal macrophages in vitro. • Autophagy induction reduces parasite internalization in macrophages. • Starved non-professional phagocytes impair parasite intracellular life cycle. • Host autophagy induction decreases infection in vitro , in ATG5-dependent manner. Trypanosoma cruzi causes Chagas disease, a neglected illness that affects millions of people worldwide, especially in Latin America. The balance between biochemical pathways triggered by the parasite and host cells response will ultimately define the progression of a life-threatening disease, justifying the efforts to understand cellular mechanisms for infection restrain. In this interaction, parasite and host cells are affected by different physiological responses as autophagy modulation, which could be under intense cellular stress, such as nutrient deprivation, hormone depletion, or infection. Autophagy is a constitutive pathway that leads to degradation of macromolecules and cellular structures and may induce cell death. In Trypanosoma cruzi infection, the relevance of host autophagy is controversial regarding in vitro parasite intracellular life cycle. In the present study, we evaluated host cell autophagy during T. cruzi infection in phagocytic and non-professional phagocytic cells. We described that the presence of the parasite increased the number of LC3 puncta, a marker for autophagy, in cardiac cells and peritoneal macrophages in vitro. The induction of host autophagy decreased infection in macrophages in early and late time-periods. We suggest that starved phagocytic cells reduced internalization, also confirmed by inert particles and dead trypomastigotes. Whereas, in cardiac cells, starvation-induced autophagy decreased lipid droplets and infection in later time-point, by reducing parasite differentiation/proliferation. In ATG5 knockout MEF cells, we confirmed our hypothesis of autophagy machinery activation during parasite internalization, increasing infection. Our data suggest that host autophagy downregulates T. cruzi infection through impairing parasite intracellular life cycle, reducing the infection in primary culture cells. [ABSTRACT FROM AUTHOR]

Published

2020

3. Trypanosoma cruzi infection of human induced pluripotent stem cell-derived cardiomyocytes: an in vitro model for drug screening for Chagas disease.

Author

da Silva Lara, Leonardo, Andrade-Lima, Leonardo, Magalhães Calvet, Claudia, Borsoi, Juliana, Lopes Alberto Duque, Thabata, Henriques-Pons, Andrea, Souza Pereira, Mirian Claudia, and Veiga Pereira, Lygia

Subjects

*CHAGAS' disease treatment, *CHAGAS' disease, *TRYPANOSOMA cruzi, *CARDIOTOXICITY, *DRUG efficacy, *PATIENTS

Abstract

Chagas disease, caused by Trypanosoma cruzi , is an important global public health problem which, despite partial efficacy of benznidazole (Bz) in acute phase, urgently needs an effective treatment. Cardiotoxicity is a major safety concern for conduction of more accurate preclinical drug screening platforms. Human induced pluripotent stem cells derived cardiomyocytes (hiPSC-CM) are a reliable model to study genetic and infectious cardiac alterations and may improve drug development. Herein, we introduce hiPSC-CM as a suitable model to study T. cruzi heart infection and to predict the safety and efficacy of anti- T. cruzi drugs. [ABSTRACT FROM AUTHOR]

Published

2018

4. ATG5 provides host protection acting as a switch in the atg8ylation cascade between autophagy and secretion.

Author

Wang, Fulong, Peters, Ryan, Jia, Jingyue, Mudd, Michal, Salemi, Michelle, Allers, Lee, Javed, Ruheena, Duque, Thabata L.A., Paddar, Masroor A., Trosdal, Einar S., Phinney, Brett, and Deretic, Vojo

Subjects

*AUTOPHAGY, *LYSOSOMES, *SECRETION, *NEUTROPHILS, *UBIQUITIN ligases, *EXTRACELLULAR vesicles, *MYELOID cells, *UBIQUITINATION

Abstract

ATG5 is a part of the E3 ligase directing lipidation of ATG8 proteins, a process central to membrane atg8ylation and canonical autophagy. Loss of Atg5 in myeloid cells causes early mortality in murine models of tuberculosis. This in vivo phenotype is specific to ATG5. Here, we show using human cell lines that absence of ATG5, but not of other ATGs directing canonical autophagy, promotes lysosomal exocytosis and secretion of extracellular vesicles and, in murine Atg5fl/fl LysM-Cre neutrophils, their excessive degranulation. This is due to lysosomal disrepair in ATG5 knockout cells and the sequestration by an alternative conjugation complex, ATG12-ATG3, of ESCRT protein ALIX, which acts in membrane repair and exosome secretion. These findings reveal a previously undescribed function of ATG5 in its host-protective role in murine experimental models of tuberculosis and emphasize the significance of the branching aspects of the atg8ylation conjugation cascade beyond the canonical autophagy. [Display omitted] • ATG5 is at a cardinal junction between canonical and noncanonical ATG conjugates • Loss of ATG5 favors a sidestep conjugate ATG12-ATG3 that sequesters ESCRT ALIX • Loss of ATG5 causes lysosomal hypersensitivity to damage and increased exocytosis • The noncanonical role of ATG5 affects neutrophils and tuberculosis pathogenesis Wang et al. describe properties of a core autophagy protein ATG5, which fall outside of its canonical autophagy functions. Loss of ATG5 dysregulates lysosomal repair, increases exocytosis and exosome release, and in neutrophils causes hyperactivation and degranulation, partly explaining the function of ATG5 in mouse models of tuberculosis. [ABSTRACT FROM AUTHOR]

Published

2023