Exploration of immunoglobulin transcriptomes from mice immunized with three-finger toxins and phospholipases A2 from the Central American coral snake, Micrurus nigrocinctus
Fecha
2017
Autores
Laustsen, Andreas Hougaard
Engmark, Mikael Gerling
Clouser, Christopher
Timberlake, Sonia
Vigneault, Francois
Gutiérrez, José María
Lomonte, Bruno
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Resumen
Snakebite envenomings represent a neglected public health issue in many parts of the
rural tropical world. Animal-derived antivenoms have existed for more than a hundred
years and are effective in neutralizing snake venom toxins when timely administered.
However, the low immunogenicity of many small but potent snake venom toxins
represents a challenge for obtaining a balanced immune response against the medically
relevant components of the venom. Here, we employ high-throughput sequencing of
the immunoglobulin (Ig) transcriptome of mice immunized with a three-finger toxin
and a phospholipase A2 from the venom of the Central American coral snake, Micrurus
nigrocinctus. Although exploratory in nature, our indicate results showed that only low
frequencies of mRNA encoding IgG isotypes, the most relevant isotype for therapeutic
purposes, were present in splenocytes of five mice immunized with 6 doses of the two
types of toxins over 90 days. Furthermore, analysis of Ig heavy chain transcripts showed
that no particular combination of variable (V) and joining (J) gene segments had been
selected in the immunization process, as would be expected after a strong humoral
immune response to a single antigen. Combined with the titration of toxin-specific
antibodies in the sera of immunized mice, these data support the low immunogenicity
of three-finger toxins and phospholipases A2 found in M. nigrocinctus venoms, and
highlight the need for future studies analyzing the complexity of antibody responses to
toxins at the molecular level.
Descripción
Palabras clave
antivenom, antibody, Micrurus, transcriptomics, Snake venom
Citación
https://peerj.com/articles/2924/