Protection of C57BL/10 mice by vaccination with association of purified proteins from Leishmania (Leishmania) amazonensis

MORA, Ana Mariela; MAYRINK, Wilson; COSTA, Roberto Teodoro da; COSTA, Carlos Alberto da; GENARO, Odair; NASCIMENTO, Evaldo

doi:10.1590/S0036-46651999000400008

In the past few years, induction of protective immunity to cutaneous leishmaniasis has been attempted by many researchers using a variety of antigenic preparations, such as living promastigotes or promastigote extracts, partially purified, or defined proteins. In this study, eleven proteins from Leishmania (Leishmania) amazonensis (LLa) with estimated molecular mass ranging from 97 to 13.5kDa were isolated by polyacrylamide gel electrophoresis and electro-elution. The proteins were associated as vaccine in different preparations with gp63 and BCG (Bacilli Calmette-Guérin). The antigenicity of these vaccines was measured by their ability to induce the production of IFN-g by lymphocyte from subjects vaccinated with Leishvacinâ . The immunogenicity was evaluated in vaccinated mice. C57BL/10 mice were vaccinated with three doses of each vaccine consisting of 30 mg of each protein at 15 days interval. One hundred mg of live BCG was only used in the first dose. Seven days after the last dose, they received a first challenge infection with 105 infective promastigotes and four months later, a second challenge was done. Two months after the second challenge, 42.86% of protection was obtained in the group of mice vaccinated with association of proteins of gp63+46+22kDa, gp63+13.5+25+42kDa, gp63+46+42kDa, gp63+66kDa, and gp63+97kDa; 57.14% of protection was demonstrated with gp63+46+97+13.5kDa, gp63+46+97kDa, gp63+46+33kDa, and 71.43% protection for gp63 plus all proteins. The vaccine of gp63+46+40kDa that did not protect the mice, despite the good specific stimulation of lymphocytes (LSI = 7.60) and 10.77UI/ml of IFN-g production. When crude extract of L. (L.) amazonensis was used with BCG a 57.14% of protection was found after the first challenge and 28.57% after the second, the same result was observed for gp63. The data obtained with the vaccines can suggest that the future vaccine probably have to contain, except the 40kDa, a cocktail of proteins that would protect mice against cutaneous leishmaniasis.

Leishmania; Proteins; Mice; Vaccine

Group of 7 mice	Vaccine components (kDa)	IFN-g (U/ml)	LSI (Ratio)
1	gp63+46+97+BCG	15.54	8.00
2	gp63+46+13.5+BCG	11.23	10.00
3	gp63+46+22+BCG	16.80	10.40
4	gp63+46+97+13.5+BCG	13.56	9.60
5	gp63+46+33+BCG	19.14	11.70
6	gp63+46+40+BCG	10.77	7.60
7	gp63+46+42+BCG	12.55	9.00
8	gp63+13.5+25+42+BCG	13.81	7.80
9	gp63+66+BCG	14.00	7.20
10	gp63+97+BCG	11.23	8.30
11	gp63+85+97+BCG	15.82	10.10
12	gp63+all proteins+BCG	14.61	8.50
13	gp63+BCG	10.08	10.20
14	LLa+BCG	13.32	10.80
15	BCG	9.16	5.10
16	PBS	5.11	1.50

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Protection of C57BL/10 mice by vaccination with association of purified proteins from Leishmania (Leishmania) amazonensis

Proteção de camundongos C57BL/10 vacinados por vacinas contituidas pelas combinações de proteínas purificadas de Leishmania (Leishmania) amazonensis

Group of 7 mice	Vaccine components (kDa)	Efficacy (%)
Group of 7 mice	Vaccine components (kDa)	143 days after first challenge	60 days after second challenge
1	gp63+46+97+BCG	57.14	57.14
2	gp63+46+13.5+BCG	57.14	28.57
3	gp63+46+22+BCG	57.14	42.86
4	gp63+46+97+13.5+BCG	57.14	57.14
5	gp63+46+33+BCG	57.14	57.14
6	gp63+46+40+BCG	00.00	00.00
7	gp63+46+42+BCG	42.86	42.86
8	gp63+13.5+25+42+BCG	42.86	42.86
9	gp63+66+BCG	42.86	42.86
10	gp63+97+BCG	42.86	42.86
11	gp63+85+97+BCG	57.14	28.57
12	gp63+all proteins+BCG	71.43	71.43
13	gp63+BCG	57.14	28.57
14	LLa+BCG	57.14	28.57
15	BCG	14.29	00.00
16	PBS	00.00	00.00