Not insertion. Knock-out.

Disrupting the serotonin synthesis pathway in the central nervous system. Pure science objective of understanding what serotonin really does. Applied science goal of developing novel methods to decrease mosquito host-seeking to prevent disease transmission.

...because of its neurological implications.

(Among other things, I'm an insomniac, so there's that.)

It would not have occurred to me, although it probably should have, that serotonin chemistry is neurologically conserved across animal species, but on reflection, it make sense that it is.

Is the hydroxylase in question fairly well conserved across animal species? It has been my pleasure to select appropriate peptides in cross species gene insertions to avoid conserved sequences.

It happens to have a eye catching "HELL" motif in its amino acid sequence that is shared from worms to us.

It is a nifty little enzyme, and serotonin is a cool molecule.

More specifically GHELLGH or something like that. coordinates an iron molecule.

...just because, well, just because...

I'm a mass spec kind of person as far as proteomics goes, and I often find myself contemplating sequences across species, as I have been peripherally involved in gene modification for genetic diseases. It comes up when one is inserting a human gene in a monkey to experiment in preclinical trials with treating genetic syndromes.

https://www.uniprot.org/uniprotkb/Q8IWU9/entry

Q8IWU9


This is the human protein, but it shares amazing conservation. I think my form is still in the uncharacterized category but better model organisms share it and are pretty close to the mosquito.

It also happens to be a beautiful, symmetry homotetramer.

A former advisor of mine told me to stay away from serotonin research because it would "make me crazy," which is a spectacular line. I love him.

Has the mosquito been fully sequenced?

An interesting question is whether the mosquito will be viable without the gene and its translation; might it not starve to death?

Based on work in Drosophila, the knockout mutants are viable.

This same mutation has been done in mice and they are also viable, just highly anxious and aggressive.

The interesting thing about this particular enzyme is it has two isoforms: one that generates serotonin in peripheral tissues, and one that solely operates in the nervous system. I'm knocking out the nervous system one.

The literature seems to suggest that dopamine circuits compensate for the missing serotonin, and there is enough in the somatic cells to prevent major developmental problems.