Publications by authors named "H Arnould"

Corruption of cellular prion protein (PrPC) function(s) at the plasma membrane of neurons is at the root of prion diseases, such as Creutzfeldt-Jakob disease and its variant in humans, and Bovine Spongiform Encephalopathies, better known as mad cow disease, in cattle. The roles exerted by PrPC, however, remain poorly elucidated. With the perspective to grasp the molecular pathways of neurodegeneration occurring in prion diseases, and to identify therapeutic targets, achieving a better understanding of PrPC roles is a priority.

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Abundant evidence has accumulated showing that fetal alcohol exposure broadly modifies DNA methylation profiles in the brain. DNA methyltransferases (DNMTs), the enzymes responsible for DNA methylation, are likely implicated in this process. However, their regulation by ethanol exposure has been poorly addressed.

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A popular method for studying the function of a given protein is to generate and characterize a suitable model deficient for its expression. For the prion protein (PrP), best known for its role in several invariably fatal neurodegenerative diseases, a natural choice, therefore, would be to undertake such studies with brain samples. We recently documented the surprising observation that PrP deficiency caused a loss or enhancement of NCAM1 polysialylation, dependent on the cell model used.

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Article Synopsis
  • A study evaluated the effects of cementless dual mobility sockets in primary total hip arthroplasty (THA) on dislocation rates, hip function, and acetabular fixation.
  • The research involved 168 patients, with a significant focus on those who had evaluations after at least 5 years post-surgery.
  • Results indicated that while the dual mobility socket generally led to pain-free mobility and solid fixation, using a long-neck option could increase the risk of intraprosthetic dislocations, necessitating revisions in some cases.
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