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In vitro generation of polysialylated cervical mucins by bacterial polysialyltransferases to counteract cytotoxicity of extracellular histones

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Neutrophil extracellular traps (NET) are formed against pathogens. However, various diseases are directly linked to this meshwork of DNA. The cytotoxic properties of extracellular histones especially seem to be an important trigger during these diseases. Furthermore, NET accumulation on implants is discussed to result in an impaired efficiency or failure, depending on the category of implant. Interestingly, mucins have been investigated as surface coatings potentially capable of reducing neutrophil adhesion. Similarly, polysialic acid was shown to inactivate the cytotoxic properties of extracellular histones. We wanted to combine the probability to decrease the adhesion of neutrophils using mucins with the capability of sialic acid polymers to counteract histone‐mediated cytotoxicity. To this end, we elongate cervical mucins using bacterial polysialyltransferases. Subsequent cell‐based experiments demonstrated the activity of elongated mucins against histone‐mediated cytotoxicity. Thus, polysialylated mucins may represent a novel component to coat implants or to combat diseases with exaggerated NET formation.
Title: In vitro generation of polysialylated cervical mucins by bacterial polysialyltransferases to counteract cytotoxicity of extracellular histones
Description:
Neutrophil extracellular traps (NET) are formed against pathogens.
However, various diseases are directly linked to this meshwork of DNA.
The cytotoxic properties of extracellular histones especially seem to be an important trigger during these diseases.
Furthermore, NET accumulation on implants is discussed to result in an impaired efficiency or failure, depending on the category of implant.
Interestingly, mucins have been investigated as surface coatings potentially capable of reducing neutrophil adhesion.
Similarly, polysialic acid was shown to inactivate the cytotoxic properties of extracellular histones.
We wanted to combine the probability to decrease the adhesion of neutrophils using mucins with the capability of sialic acid polymers to counteract histone‐mediated cytotoxicity.
To this end, we elongate cervical mucins using bacterial polysialyltransferases.
Subsequent cell‐based experiments demonstrated the activity of elongated mucins against histone‐mediated cytotoxicity.
Thus, polysialylated mucins may represent a novel component to coat implants or to combat diseases with exaggerated NET formation.

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