Rabbit serum against K1 peptide, an immunogenic epitope of the Trypanosoma cruzi KMP-11, decreases parasite invasion to cells

Soto, Juan C. Diaz; Lasso, Paola; Guzmán, Fanny; Forero-Shelton, Manu; Thomas, M. Carmen; López, Manuel Carlos; Guhl, Felipe; Cuéllar, Adriana; Puerta, Concepción J.; González, John Mario

doi:10.1016/j.actatropica.2012.05.015

Cited by 5 publications

(9 citation statements)

References 38 publications

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“…The number of infected cells was estimated by counting 200 randomly distributed cells using 100 X magnification in a light microscope. Three independent experiments were performed in duplicate [ 31 ].…”

Section: Methodsmentioning

confidence: 99%

A terpenoid-rich extract from Clethra fimbriata exhibits anti-Trypanosoma cruzi activity and induces T cell cytokine production

Pardo-Rodriguez

Lasso

Mateus

et al. 2022

Heliyon

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Section: Methodsmentioning

confidence: 99%

A terpenoid-rich extract from Clethra fimbriata exhibits anti-Trypanosoma cruzi activity and induces T cell cytokine production

Pardo-Rodriguez

Lasso

Mateus

et al. 2022

Heliyon

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“…As we have previously described (Diaz-Soto et al, 2012), polyclonal antibodies against TcTLE peptide are able to bind to the native KMP-11 on T. cruzi's trypomastigote surface and reduce the parasite's capacity to infect susceptible Vero cells. However, the relatively low antibody titers, although significant for immunization with a 9-mer peptide alone, limited further functional analysis.…”

Section: Discussionmentioning

confidence: 84%

“…We have previously shown that immunization of rabbits with the TcTLE peptide produces polyclonal antibodies that recognize live forms of T. cruzi and reduce parasite invasion in Vero cells (Diaz-Soto et al, 2012). However, the low antibody titers obtained prevented further assessment of their potential functional properties.…”

Section: Introductionmentioning

confidence: 97%

Altering the motility of Trypanosoma cruzi with rabbit polyclonal anti-peptide antibodies reduces infection to susceptible mammalian cells

Finkelsztein

Soto

Vargas-Zambrano

et al. 2015

Experimental Parasitology

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“…%, SD = 0.07). In addition, MP-FLU-specific CD8 + T cells were predominantly effector memory T cells (T EM : CCR7 -CD62L -), distributed in the early or intermediate/late differentiation stages, producing IL-2, IFN-g, CD107a/b, and perforin without showing significant differences when compared with those from HD (Lasso et al, 2012). In all, these data support the hypothesis that parasite antigens induce a specific CD8 + T cell dysfunctionality in terms of reduced proliferation capacity and a prolonged activation state.…”

Section: Deciphering Cd8 + T Cells In Chagas Diseasementioning

confidence: 97%

“…It was also studied whether the alteration in the functionality of CD8 + T cells was nonspecific or specific to parasite antigens; we studied the CD8 + T cell response of CCP against an antigen of another microorganism. In this case, the MP-FLU peptide (GILGFVFTL) derived from the influenza virus, which is also restricted to HLA-A2 (Lasso et al, 2012). The results showed that MP-FLU peptide-specific CD8 + T cells presented similar frequencies in the five HLA-A2 + HD (0.12-0.29%, mean 0.17%, SD = 0.07) and the 13 HLA-A2 + CCP (0.12-0.37%, mean 0.21.…”

Section: Deciphering Cd8 + T Cells In Chagas Diseasementioning

confidence: 99%

Trypanosoma cruzi-specific CD8+ T cells and other immunological hallmarks in chronic Chagas cardiomyopathy: Two decades of research

Puerta

Cuéllar

Lasso

et al. 2023

Front. Cell. Infect. Microbiol.

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Trypanosoma cruzi, the causal agent of Chagas disease, has coexisted with humans for thousands of years. Therefore, the parasite has developed several mechanisms of antigenic variability that has allowed it to live inside the cells and evade the host immune response. Since T. cruzi displays an intracellular cycle-stage, our research team focused on providing insights into the CD8+ T cells immune response in chronic Chagas cardiomyopathy. We began our work in the 2000s studying parasite antigens that induce natural immune responses such as the KMP11 protein and TcTLE, its N-terminal derived peptide. Different approaches allowed us to reveal TcTLE peptide as a promiscuous CD8+ T cell epitope, able of inducing multifunctional cellular immune responses and eliciting a humoral response capable of decreasing parasite movement and infective capacity. Next, we demonstrated that as the disease progresses, total CD8+ T cells display a dysfunctional state characterized by a prolonged hyper-activation state along with an increase of inhibitory receptors (2B4, CD160, PD-1, TIM-3, CTLA-4) expression, an increase of specific terminal effector T cells (TTE), a decrease of proliferative capacity, a decrease of stem cell memory (TSCM) frequency, and a decrease of CD28 and CD3ζ expression. Thus, parasite-specific CD8+ T cells undergo clonal exhaustion, distinguished by an increase in late-differentiated cells, a mono-functional response, and enhanced expression of inhibitory receptors. Finally, it was found that anti-parasitic treatment induces an improved CD8+ T cell response in asymptomatic individuals, and a mouse animal model led us to establish a correlation between the quality of the CD8+ T cell responses and the outcome of chronic infection. In the future, using OMICs strategies, the identification of the specific cellular signals involved in disease progression will provide an invaluable resource for discovering new biomarkers of progression or new vaccine and immunotherapy strategies. Also, the inclusion of the TcTLE peptide in the rational design of epitope-based vaccines, the development of immunotherapy strategies using TSCM or the blocking of inhibitory receptors, and the use of the CD8+ T cell response quality to follow treatments, immunotherapies or vaccines, all are alternatives than could be explored in the fight against Chagas disease.

show abstract

Rabbit serum against K1 peptide, an immunogenic epitope of the Trypanosoma cruzi KMP-11, decreases parasite invasion to cells

Cited by 5 publications

References 38 publications

A terpenoid-rich extract from Clethra fimbriata exhibits anti-Trypanosoma cruzi activity and induces T cell cytokine production

A terpenoid-rich extract from Clethra fimbriata exhibits anti-Trypanosoma cruzi activity and induces T cell cytokine production

Altering the motility of Trypanosoma cruzi with rabbit polyclonal anti-peptide antibodies reduces infection to susceptible mammalian cells

Trypanosoma cruzi-specific CD8+ T cells and other immunological hallmarks in chronic Chagas cardiomyopathy: Two decades of research

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