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

Eli J. Finkelsztein; Juan C. Diaz-Soto; Juan C. Vargas-Zambrano; Elizabeth Suesca; Fanny Guzmán; Manuel C. López; M. Carmen Thomas; Manu Forero-Shelton; Adriana Cuellar; Concepción J. Puerta; John M. González

doi:10.1016/j.exppara.2015.01.007

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

Eli J. Finkelsztein, Juan C. Diaz-Soto, Juan C. Vargas-Zambrano, Elizabeth Suesca, Fanny Guzmán, Manuel C. López, M. Carmen Thomas, Manu Forero-Shelton, Adriana Cuellar, Concepción J. Puerta, John M. González

Department of Microbiology

Research output: Contribution to journal › Article › peer-review

12 Scopus citations

Abstract

Trypanosoma cruzi's trypomastigotes are highly active and their incessant motility seems to be important for mammalian host cell infection. The kinetoplastid membrane protein-11 (KMP-11) is a protein expressed in all parasite stages, which induces a cellular and humoral immune response in the infected host, and is hypothesized to participate in the parasite's motility. An N-terminal peptide from KMP-11, termed K1 or TcTLE, induced polyclonal antibodies that inhibit parasitic invasion of Vero cells. The goal of this study was to evaluate the motility and infectivity of T. cruzi when exposed to polyclonal anti-TcTLE antibodies. Rabbits were immunized with TcTLE peptide along with FIS peptide as an immunomodulator. ELISA assay results showed that post-immunization sera contained high titers of polyclonal anti-TcTLE antibodies, which were also reactive against the native KMP-11 protein and live parasites as detected by immunofluorescence and flow cytometry assays. Trypomastigotes of T. cruzi were incubated with pre- or post-immunization sera, and infectivity to human astrocytes was assessed by Giemsa staining/light microscope and flow cytometry using carboxyfluorescein diacetate succinimidyl ester (CFSE) labeled parasites. T. cruzi infection in astrocytes decreased approximately by 30% upon incubation with post-immunization sera compared with pre-immunization sera. Furthermore, trypomastigotes were recorded by video microscopy and the parasite's flagellar speed was calculated by tracking the flagella. Trypomastigotes exposed to post-immunization sera had qualitative alterations in motility and significantly slower flagella (45.5 μm/s), compared with those exposed to pre-immunization sera (69.2 μm/s). In summary, polyclonal anti-TcTLE serum significantly reduced the parasite's flagellar speed and cell infectivity. These findings support that KMP-11 could be important for parasite motility, and that by targeting its N-terminal peptide infectivity can be reduced.

Original language	English
Pages (from-to)	36-43
Number of pages	8
Journal	Experimental Parasitology
Volume	150
DOIs	https://doi.org/10.1016/j.exppara.2015.01.007
State	Published - 01 Mar 2015

Keywords

Anti-peptide antibodies
Chagas disease
Flow cytometry
Trypanosoma cruzi

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.exppara.2015.01.007

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Finkelsztein, E. J., Diaz-Soto, J. C., Vargas-Zambrano, J. C., Suesca, E., Guzmán, F., López, M. C., Thomas, M. C., Forero-Shelton, M., Cuellar, A., Puerta, C. J., & González, J. M. (2015). Altering the motility of Trypanosoma cruzi with rabbit polyclonal anti-peptide antibodies reduces infection to susceptible mammalian cells. Experimental Parasitology, 150, 36-43. https://doi.org/10.1016/j.exppara.2015.01.007

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

abstract = "Trypanosoma cruzi's trypomastigotes are highly active and their incessant motility seems to be important for mammalian host cell infection. The kinetoplastid membrane protein-11 (KMP-11) is a protein expressed in all parasite stages, which induces a cellular and humoral immune response in the infected host, and is hypothesized to participate in the parasite's motility. An N-terminal peptide from KMP-11, termed K1 or TcTLE, induced polyclonal antibodies that inhibit parasitic invasion of Vero cells. The goal of this study was to evaluate the motility and infectivity of T. cruzi when exposed to polyclonal anti-TcTLE antibodies. Rabbits were immunized with TcTLE peptide along with FIS peptide as an immunomodulator. ELISA assay results showed that post-immunization sera contained high titers of polyclonal anti-TcTLE antibodies, which were also reactive against the native KMP-11 protein and live parasites as detected by immunofluorescence and flow cytometry assays. Trypomastigotes of T. cruzi were incubated with pre- or post-immunization sera, and infectivity to human astrocytes was assessed by Giemsa staining/light microscope and flow cytometry using carboxyfluorescein diacetate succinimidyl ester (CFSE) labeled parasites. T. cruzi infection in astrocytes decreased approximately by 30% upon incubation with post-immunization sera compared with pre-immunization sera. Furthermore, trypomastigotes were recorded by video microscopy and the parasite's flagellar speed was calculated by tracking the flagella. Trypomastigotes exposed to post-immunization sera had qualitative alterations in motility and significantly slower flagella (45.5 μm/s), compared with those exposed to pre-immunization sera (69.2 μm/s). In summary, polyclonal anti-TcTLE serum significantly reduced the parasite's flagellar speed and cell infectivity. These findings support that KMP-11 could be important for parasite motility, and that by targeting its N-terminal peptide infectivity can be reduced.",

keywords = "Anti-peptide antibodies, Chagas disease, Flow cytometry, Trypanosoma cruzi",

author = "Finkelsztein, {Eli J.} and Diaz-Soto, {Juan C.} and Vargas-Zambrano, {Juan C.} and Elizabeth Suesca and Fanny Guzm{\'a}n and L{\'o}pez, {Manuel C.} and Thomas, {M. Carmen} and Manu Forero-Shelton and Adriana Cuellar and Puerta, {Concepci{\'o}n J.} and Gonz{\'a}lez, {John M.}",

note = "Publisher Copyright: {\textcopyright} 2015 Elsevier Inc.",

year = "2015",

month = mar,

day = "1",

doi = "10.1016/j.exppara.2015.01.007",

language = "English",

volume = "150",

pages = "36--43",

journal = "Experimental Parasitology",

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Finkelsztein, EJ, Diaz-Soto, JC, Vargas-Zambrano, JC, Suesca, E, Guzmán, F, López, MC, Thomas, MC, Forero-Shelton, M, Cuellar, A, Puerta, CJ & González, JM 2015, 'Altering the motility of Trypanosoma cruzi with rabbit polyclonal anti-peptide antibodies reduces infection to susceptible mammalian cells', Experimental Parasitology, vol. 150, pp. 36-43. https://doi.org/10.1016/j.exppara.2015.01.007

TY - JOUR

T1 - Altering the motility of Trypanosoma cruzi with rabbit polyclonal anti-peptide antibodies reduces infection to susceptible mammalian cells

AU - Finkelsztein, Eli J.

AU - Diaz-Soto, Juan C.

AU - Vargas-Zambrano, Juan C.

AU - Suesca, Elizabeth

AU - Guzmán, Fanny

AU - López, Manuel C.

AU - Thomas, M. Carmen

AU - Forero-Shelton, Manu

AU - Cuellar, Adriana

AU - Puerta, Concepción J.

AU - González, John M.

PY - 2015/3/1

Y1 - 2015/3/1

N2 - Trypanosoma cruzi's trypomastigotes are highly active and their incessant motility seems to be important for mammalian host cell infection. The kinetoplastid membrane protein-11 (KMP-11) is a protein expressed in all parasite stages, which induces a cellular and humoral immune response in the infected host, and is hypothesized to participate in the parasite's motility. An N-terminal peptide from KMP-11, termed K1 or TcTLE, induced polyclonal antibodies that inhibit parasitic invasion of Vero cells. The goal of this study was to evaluate the motility and infectivity of T. cruzi when exposed to polyclonal anti-TcTLE antibodies. Rabbits were immunized with TcTLE peptide along with FIS peptide as an immunomodulator. ELISA assay results showed that post-immunization sera contained high titers of polyclonal anti-TcTLE antibodies, which were also reactive against the native KMP-11 protein and live parasites as detected by immunofluorescence and flow cytometry assays. Trypomastigotes of T. cruzi were incubated with pre- or post-immunization sera, and infectivity to human astrocytes was assessed by Giemsa staining/light microscope and flow cytometry using carboxyfluorescein diacetate succinimidyl ester (CFSE) labeled parasites. T. cruzi infection in astrocytes decreased approximately by 30% upon incubation with post-immunization sera compared with pre-immunization sera. Furthermore, trypomastigotes were recorded by video microscopy and the parasite's flagellar speed was calculated by tracking the flagella. Trypomastigotes exposed to post-immunization sera had qualitative alterations in motility and significantly slower flagella (45.5 μm/s), compared with those exposed to pre-immunization sera (69.2 μm/s). In summary, polyclonal anti-TcTLE serum significantly reduced the parasite's flagellar speed and cell infectivity. These findings support that KMP-11 could be important for parasite motility, and that by targeting its N-terminal peptide infectivity can be reduced.

AB - Trypanosoma cruzi's trypomastigotes are highly active and their incessant motility seems to be important for mammalian host cell infection. The kinetoplastid membrane protein-11 (KMP-11) is a protein expressed in all parasite stages, which induces a cellular and humoral immune response in the infected host, and is hypothesized to participate in the parasite's motility. An N-terminal peptide from KMP-11, termed K1 or TcTLE, induced polyclonal antibodies that inhibit parasitic invasion of Vero cells. The goal of this study was to evaluate the motility and infectivity of T. cruzi when exposed to polyclonal anti-TcTLE antibodies. Rabbits were immunized with TcTLE peptide along with FIS peptide as an immunomodulator. ELISA assay results showed that post-immunization sera contained high titers of polyclonal anti-TcTLE antibodies, which were also reactive against the native KMP-11 protein and live parasites as detected by immunofluorescence and flow cytometry assays. Trypomastigotes of T. cruzi were incubated with pre- or post-immunization sera, and infectivity to human astrocytes was assessed by Giemsa staining/light microscope and flow cytometry using carboxyfluorescein diacetate succinimidyl ester (CFSE) labeled parasites. T. cruzi infection in astrocytes decreased approximately by 30% upon incubation with post-immunization sera compared with pre-immunization sera. Furthermore, trypomastigotes were recorded by video microscopy and the parasite's flagellar speed was calculated by tracking the flagella. Trypomastigotes exposed to post-immunization sera had qualitative alterations in motility and significantly slower flagella (45.5 μm/s), compared with those exposed to pre-immunization sera (69.2 μm/s). In summary, polyclonal anti-TcTLE serum significantly reduced the parasite's flagellar speed and cell infectivity. These findings support that KMP-11 could be important for parasite motility, and that by targeting its N-terminal peptide infectivity can be reduced.

KW - Anti-peptide antibodies

KW - Chagas disease

KW - Flow cytometry

KW - Trypanosoma cruzi

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U2 - 10.1016/j.exppara.2015.01.007

DO - 10.1016/j.exppara.2015.01.007

M3 - Article

C2 - 25633439

AN - SCOPUS:84922418857

SN - 0014-4894

VL - 150

SP - 36

EP - 43

JO - Experimental Parasitology

JF - Experimental Parasitology

ER -

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

Abstract

Keywords

UN SDGs

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