Research study identifies a new therapeutic target for Alzheimer鈥檚 disease

Research from the Neuroscience Institute identifies the impact of a reduction in astrocytes in the hexokinase 1 (HK1) enzyme in Alzheimer鈥檚 disease, paving a new pathway for potential treatments.

image of astrocytes under microscope
  • Research undertaken by Dr Simon Bell and led by Professor Heather Mortiboys from the Neuroscience Institute has identified a specific enzyme that impacts glucose metabolism and cell function in Alzheimer鈥檚 disease
  • The findings of this show a reduction of astrocytes in hexokinase 1 (HK1) in the early stages of Alzheimer鈥檚 disease and identify this enzyme as a new therapeutic target for potential treatments

Worldwide, at least 50 million people are believed to be living with a form of dementia.

Alzheimer's disease is the most common type of dementia. It is a progressive and irreversible neurodegenerative disorder that primarily affects memory and cognitive functions. Symptoms include memory loss that disrupts daily life, poor judgement and taking longer to complete normal daily tasks. There is currently no cure.

The most common form of Alzheimer鈥檚 disease is called sporadic Alzheimer鈥檚 disease which occurs due to a complex combination of genes, environment and lifestyle. It has no specific family link. 

Astrocytes are a subtype of important cells that make up the majority of cells in the nervous system. They perform many functions including providing nutrients, support, and insulation for neurons. Early in Alzheimer鈥檚 disease, it has been shown that astrocytes have problems with their metabolism and aren鈥檛 able to process information properly, impacting the energy used to help neurons function effectively. 

鈥淢ost people focus on neurons, but there are actually more astrocytes in the brain than neurons. Once the metabolism of astrocytes becomes perturbed, then the astrocyte definitely will not be able to provide as much support to neurons鈥 explains Professor Heather Mortiboys from the Neuroscience Institute.

undertaken by Dr Simon Bell from the Neuroscience Institute at the University of 91直播 was the first to identify the impact of damaged astrocytes in sporadic Alzheimer鈥檚 disease on cellular power plants known as the mitochondria. The study found that damaged astrocytes in Alzheimer鈥檚 disease have less energy production and generate more stress on the mitochondria. 

Crucially, the study discovered that a key enzyme called hexokinase 1 (HK1) was lower in astrocytes from people with sporadic Alzheimer's disease. The study revealed that by boosting this enzyme, it was possible to improve the energy of astrocytes in sporadic Alzheimer鈥檚 disease and reduce the negative impact of abnormal astrocytes.

The study was undertaken by Dr Simon Bell and led by Professor Heather Mortiboys. The study involved many researchers including Hollie Wareing, Francesco Capriglia, Rachel Hughes, Katy Barnes, Alexander Hamshaw, Dr Liam Adair, Allan Shaw, Alicja Olejnik, Suman De, Elizabeth New, Professor Dame Pamela J. Shaw, Dr Matteo De Marco, Professor Annalena Venneri, Dr Daniel J. Blackburn, and Laura Ferraiuolo.

鈥淔or this study, we took samples from patients with sporadic Alzheimer鈥檚 disease via a skin biopsy and grew skin cells, or fibroblasts, in the lab. We then used reprogramming techniques to turn them into stem cells and differentiate them into astrocytes鈥 explains Professor Heather Mortiboys.

鈥淲hen comparing the astrocytes between sporadic Alzheimer鈥檚 and familial Alzheimer鈥檚, we found key changes in the mitochondria. As well as being a different shape and size, there are also changes in the glycolytic pathways which means the astrocytes have an overall energy deficit. The study highlights the different mechanisms at play between sporadic and familial Alzheimer鈥檚 and how boosting HK1 could improve cell metabolism in early Alzheimer鈥檚鈥 she adds.

The research suggests that problems in astrocyte metabolism may occur early in Alzheimer鈥檚 disease, but and highlights the potential role of HK1 in these processes.

This research was funded by Wellcome 4ward North, ARUK Yorkshire Network Centre Small Grant Scheme, ARUK Preparatory Clinical Fellowship Scheme, Academy of Medical Sciences Starter Grants for Clinical Lecturers Scheme, Parkinson鈥檚 UK, Michael J Fox Foundation, Australian Research Council, European Union Seventh Framework Programme and the NIHR 91直播 Biomedical Research Centre award.

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