Your search keyword '"More, John"' showing total 2 results

1. Functional effects of haemoglobin can be rescued by haptoglobin in an in vitro model of subarachnoid haemorrhage.

Author

Warming, Hannah, Deinhardt, Katrin, Garland, Patrick, More, John, Bulters, Diederik, Galea, Ian, and Vargas‐Caballero, Mariana

Subjects

SUBARACHNOID hemorrhage, HAPTOGLOBINS, THROMBOSIS, HEMOGLOBINS, CELL physiology, SUBARACHNOID space

Abstract

During subarachnoid haemorrhage, a blood clot forms in the subarachnoid space releasing extracellular haemoglobin (Hb), which causes oxidative damage and cell death in surrounding tissues. High rates of disability and cognitive decline in SAH survivors are attributed to loss of neurons and functional connections during secondary brain injury. Haptoglobin sequesters Hb for clearance, but this scavenging system is overwhelmed after a haemorrhage. Whilst exogenous haptoglobin application can attenuate cytotoxicity of Hb in vitro and in vivo, the functional effects of sub‐lethal Hb concentrations on surviving neurons and whether cellular function can be protected with haptoglobin treatment remain unclear. Here we use cultured neurons to investigate neuronal health and function across a range of Hb concentrations to establish the thresholds for cellular damage and investigate synaptic function. Hb impairs ATP concentrations and cytoskeletal structure. At clinically relevant but sub‐lethal Hb concentrations, we find that synaptic AMPAR‐driven currents are reduced, accompanied by a reduction in GluA1 subunit expression. Haptoglobin co‐application can prevent these deficits by scavenging free Hb to reduce it to sub‐threshold concentrations and does not need to be present at stoichiometric amounts to achieve efficacy. Haptoglobin itself does not impair measures of neuronal health and function at any concentration tested. Our data highlight a role for Hb in modifying synaptic function in surviving neurons, which may link to impaired cognition or plasticity after SAH and support the development of haptoglobin as a therapy for subarachnoid haemorrhage. [ABSTRACT FROM AUTHOR]

Published

2023

2. Neurofilament light predicts neurological outcome after subarachnoid haemorrhage.

Author

Garland, Patrick, Morton, Matt, Zolnourian, Ardalan, Durnford, Andrew, Gaastra, Ben, Toombs, Jamie, Heslegrave, Amanda J, More, John, Zetterberg, Henrik, Bulters, Diederik O, and Galea, Ian

Subjects

SUBARACHNOID hemorrhage, BIOMARKERS, CYTOPLASMIC filaments, SERUM albumin, TREATMENT effectiveness

Abstract

To improve outcome prediction following subarachnoid haemorrhage (SAH), we sought a biomarker integrating early brain injury and multiple secondary pathological processes in a prospective study of 42 non-traumatic SAH patients and 19 control individuals. Neurofilament light (NF-L) was elevated in CSF and serum following SAH. CSF and serum NF-L on Days 1-3 post-SAH strongly predicted modified Rankin score at 6 months, independent of World Federation of Neurosurgical Societies (WFNS) score. NF-L from Day 4 onwards also had a profound impact on outcome. To link NF-L to a SAH-specific pathological process, we investigated NF-L's relationship with extracellular haemoglobin. Most CSF haemoglobin was not complexed with haptoglobin, yet was able to be bound by exogenous haptoglobin i.e. haemoglobin was scavengeable. CSF scavengeable haemoglobin was strongly predictive of subsequent CSF NF-L. Next, we investigated NF-L efflux from the brain after SAH. Serum and CSF NF-L correlated positively. The serum/CSF NF-L ratio was lower in SAH versus control subjects, in keeping with glymphatic efflux dysfunction after SAH. CSF/serum albumin ratio was increased following SAH versus controls. The serum/CSF NF-L ratio correlated negatively with the CSF/serum albumin ratio, indicating that transfer of the two proteins across the blood-brain interface is dissociated. In summary, NF-L is a strong predictive marker for SAH clinical outcome, adding value to the WFNS score, and is a promising surrogate end point in clinical trials. [ABSTRACT FROM AUTHOR]

Published

2021