LAG3 is not expressed in human and murine neurons and does not modulate α-synucleinopathies.
Marc EmmeneggerElena De CeccoMarian Hruska-PlochanTimo EningerMatthias M SchneiderMelanie BarthElena TantardiniPierre de RossiMehtap BaciogluRebekah G LangstonAlice KaganovichNora Bengoa-VergnioryAndrès Gonzalez-GuerraMerve AvarDaniel HeinzerRegina ReimannLisa M HäslerTherese W HerlingNaunehal S MatharuNatalie LandeckKelvin C LukRonald MelkiPhilipp J KahleSimone HornemannTuomas P J KnowlesMark R CooksonMagdalini PolymenidouMathias JuckerAdriano AguzziPublished in: EMBO molecular medicine (2021)
While the initial pathology of Parkinson's disease and other α-synucleinopathies is often confined to circumscribed brain regions, it can spread and progressively affect adjacent and distant brain locales. This process may be controlled by cellular receptors of α-synuclein fibrils, one of which was proposed to be the LAG3 immune checkpoint molecule. Here, we analysed the expression pattern of LAG3 in human and mouse brains. Using a variety of methods and model systems, we found no evidence for LAG3 expression by neurons. While we confirmed that LAG3 interacts with α-synuclein fibrils, the specificity of this interaction appears limited. Moreover, overexpression of LAG3 in cultured human neural cells did not cause any worsening of α-synuclein pathology ex vivo. The overall survival of A53T α-synuclein transgenic mice was unaffected by LAG3 depletion, and the seeded induction of α-synuclein lesions in hippocampal slice cultures was unaffected by LAG3 knockout. These data suggest that the proposed role of LAG3 in the spreading of α-synucleinopathies is not universally valid.