International Journal of Molecular Sciences (Sep 2023)

Interaction of Substrates with γ-Secretase at the Level of Individual Transmembrane Helices—A Methodological Approach

  • Theresa M. Pauli,
  • Ayse Julius,
  • Francesco Costa,
  • Sabine Eschrig,
  • Judith Moosmüller,
  • Lea Fischer,
  • Christoph Schanzenbach,
  • Fabian C. Schmidt,
  • Martin Ortner,
  • Dieter Langosch

DOI
https://doi.org/10.3390/ijms241814396
Journal volume & issue
Vol. 24, no. 18
p. 14396

Abstract

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Intramembrane proteases, such as γ secretase, typically recruit multiple substrates from an excess of single-span membrane proteins. It is currently unclear to which extent substrate recognition depends on specific interactions of their transmembrane domains (TMDs) with TMDs of a protease. Here, we investigated a large number of potential pairwise interactions between TMDs of γ secretase and a diverse set of its substrates using two different configurations of BLaTM, a genetic reporter system. Our results reveal significant interactions between TMD2 of presenilin, the enzymatic subunit of γ secretase, and the TMD of the amyloid precursor protein, as well as of several other substrates. Presenilin TMD2 is a prime candidate for substrate recruitment, as has been shown from previous studies. In addition, the amyloid precursor protein TMD enters interactions with presenilin TMD 4 as well as with the TMD of nicastrin. Interestingly, the Gly-rich interfaces between the amyloid precursor protein TMD and presenilin TMDs 2 and 4 are highly similar to its homodimerization interface. In terms of methodology, the economics of the newly developed library-based method could prove to be a useful feature in related future work for identifying heterotypic TMD−TMD interactions within other biological contexts.

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