Neuroimaging, Urinary, and Plasma Biomarkers of Treatment Response in Huntington's Disease: Preclinical Evidence with the p75NTR Ligand LM11A-31

Simmons, Danielle A.; Mills, Brian D.; Butler, Robert R.; Kuan, Jason; McHugh, Tyne L.M.; Akers, Carolyn; Zhou, Jun; Syriani, Wassim; Grouban, Maged; Zeineh, Michael; Longo, Frank M.

doi:10.1007/s13311-021-01023-8

Cited by 20 publications

(11 citation statements)

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“…The follow-up of the BEL-AGE cohort in the next years will hopefully help to answer this open question. In addition to the possibility of p75 NTR as an early diagnostic biomarker, its role could be extended to disease progression ( Shepheard et al, 2017 ), and also be of interest as a pharmacodynamic biomarker to assess the effect of treatment, which is lacking in multiple neurological and psychiatric diseases ( Simmons et al, 2021 ). These latter possibilities have been extensively discussed by Shepheard et al (2017) and Simmons et al (2021) and were also discussed in a recent meta-analysis by Shi et al (2021) .…”

Section: Discussionmentioning

confidence: 99%

“…The present study identified high p75 NTR levels in 15% of the BEL-AGE individuals. The p75 NTR receptor is recently being proposed as a diagnostic biomarker of Alzheimer's disease in serum (Jiao et al, 2015), and was also proposed as a prognostic, disease progression and potential pharmacodynamic biomarker for ALS and Huntington's disease in urine, with increase in p75 NTR ECD happening prior to symptoms appearance in ALS (Shepheard et al, 2014(Shepheard et al, , 2017Shi et al, 2021;Simmons et al, 2021). Whether this predictive pattern is specific to these diseases remains unknown.…”

Section: P75 Ntr Extracellular Domain As a Biomarkermentioning

confidence: 99%

“…Upon activation, the p75 NTR receptor undergoes shedding, causing its extracellular domain (ECD) to be released into circulation ( Bergmeier et al, 2004 ; Weskamp et al, 2004 ; Duerschmied et al, 2009 ; Skeldal et al, 2011 ). Interestingly, elevated circulating p75 NTR ECD levels are observed in Alzheimer’s disease and major depressive disorders ( Zhou et al, 2013 ; Jiao et al, 2015 ), while high urinary p75 NTR levels are reported in amyotrophic lateral sclerosis (ALS) and Huntington’s disease patients ( Shepheard et al, 2014 , 2017 ; Jia et al, 2017 ; Simmons et al, 2021 ). Conversely, reduced circulating levels are reported in schizophrenia, and bipolar mania ( Zakharyan et al, 2014 ; Chen et al, 2017 ).…”

Section: Introductionmentioning

confidence: 99%

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Clinical Correlates Identify ProBDNF and Thrombo-Inflammatory Markers as Key Predictors of Circulating p75NTR Extracellular Domain Levels in Older Adults

Fleury

Schnitzer

Ledoux-Hutchinson

et al. 2022

Front. Aging Neurosci.

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The p75NTR receptor binds all neurotrophins and is mostly known for its role in neuronal survival and apoptosis. Recently, the extracellular domain (ECD) of p75NTR has been reported in plasma, its levels being dysregulated in numerous neurological diseases. However, the factors associated with p75NTR ECD levels remain unknown. We investigated clinical correlates of plasma p75NTR ECD levels in older adults without clinically manifested neurological disorders. Circulating p75NTR levels were measured by enzyme-linked immunosorbent assay in plasma obtained from participants in the BEL-AGE cohort (n = 1,280). Determinants of plasma p75NTR ECD levels were explored using linear and non-linear statistical models. Plasma p75NTR ECD levels were higher in male participants; were positively correlated with circulating concentrations of pro-brain-derived neurotrophic factor, and inflammatory markers interleukin-6 and CD40 Ligand; and were negatively correlated with the platelet activation marker P-selectin. While most individuals had p75NTR levels ranging from 43 to 358 pg/ml, high p75NTR levels reaching up to 9,000 pg/ml were detectable in a subgroup representing 15% of the individuals studied. In this cohort of older adults without clinically manifested neurological disorders, there was no association between plasma p75NTR ECD levels and cognitive performance, as assessed by the Montreal Cognitive Assessment score. The physiological relevance of high p75NTR ECD levels in plasma warrants further investigation. Further research assessing the source of circulating p75NTR is needed for a deeper understanding of the direction of effect, and to investigate whether high p75NTR ECD levels are predictive biomarkers or consequences of neuropathology.

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Section: Discussionmentioning

confidence: 99%

Section: P75 Ntr Extracellular Domain As a Biomarkermentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Clinical Correlates Identify ProBDNF and Thrombo-Inflammatory Markers as Key Predictors of Circulating p75NTR Extracellular Domain Levels in Older Adults

Fleury

Schnitzer

Ledoux-Hutchinson

et al. 2022

Front. Aging Neurosci.

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“…Among them, because of the leakage of CNS molecules through the BBB, blood represents a reliable source of several biomarkers, such as NfL [ 27 ]. Other biofluids have been tested, such as urine , from which Simmons et al, 2021 [ 37 ] could detect higher p75NTR in HD mice compared to controls. Saliva was demonstrated to contain detectable levels of tHTT, correlating with some HD clinical measures [ 38 ] and feces was used to detect bacterial alterations related to clinical features [ 39 ].…”

Section: Current Biomarkers In Huntington’s Diseasementioning

confidence: 99%

“…In search of other sources of accessible biofluids, several studies started to explore the presence of possible biomarkers in the urine of R6/2 HD mouse models. Indeed, the levels of p75 NTR were increased in R6/2 mice compared to WT mice urinary levels [ 37 ]. p75 NTR was already shown to play a role in memory dysfunction in HD patients [ 43 ] and to be altered in HD patients’ striatum [ 44 ].…”

Section: Current Biomarkers In Huntington’s Diseasementioning

confidence: 99%

Current Diagnostic Methods and Non-Coding RNAs as Possible Biomarkers in Huntington’s Disease

Pellegrini

Bergonzoni

Perrone

et al. 2022

Genes

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Whether as a cause or a symptom, RNA transcription is recurrently altered in pathologic conditions. This is also true for non-coding RNAs, with regulatory functions in a variety of processes such as differentiation, cell identity and metabolism. In line with their increasingly recognized roles in cellular pathways, RNAs are also currently evaluated as possible disease biomarkers. They could be informative not only to follow disease progression and assess treatment efficacy in clinics, but also to aid in the development of new therapeutic approaches. This is especially important for neurological and genetic disorders, where the administration of appropriate treatment during the disease prodromal stage could significantly delay, if not halt, disease progression. In this review we focus on the current status of biomarkers in Huntington’s Disease (HD), a fatal hereditary and degenerative disease condition. First, we revise the sources and type of wet biomarkers currently in use. Then, we explore the feasibility of different RNA types (miRNA, ncRNA, circRNA) as possible biomarker candidates, discussing potential advantages, disadvantages, sources of origin and the ongoing investigations on this topic.

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Ex vivo 100 μm isotropic diffusion MRI‐based tractography of connectivity changes in the end‐stage R6/2 mouse model of Huntington's disease

et al. 2022

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BackgroundHuntington's disease is a progressive neurodegenerative disorder. Brain atrophy, as measured by volumetric magnetic resonance imaging (MRI), is a downstream consequence of neurodegeneration, but microstructural changes within brain tissue are expected to precede this volumetric decline. The tissue microstructure can be assayed non‐invasively using diffusion MRI, which also allows a tractographic analysis of brain connectivity.MethodsWe here used ex vivo diffusion MRI (11.7 T) to measure microstructural changes in different brain regions of end‐stage (14 weeks of age) wild type and R6/2 mice (male and female) modeling Huntington's disease. To probe the microstructure of different brain regions, reduce partial volume effects and measure connectivity between different regions, a 100 μm isotropic voxel resolution was acquired.ResultsAlthough fractional anisotropy did not reveal any difference between wild‐type controls and R6/2 mice, mean, axial, and radial diffusivity were increased in female R6/2 mice and decreased in male R6/2 mice. Whole brain streamlines were only reduced in male R6/2 mice, but streamline density was increased. Region‐to‐region tractography indicated reductions in connectivity between the cortex, hippocampus, and thalamus with the striatum, as well as within the basal ganglia (striatum—globus pallidus—subthalamic nucleus—substantia nigra—thalamus).ConclusionsBiological sex and left/right hemisphere affected tractographic results, potentially reflecting different stages of disease progression. This proof‐of‐principle study indicates that diffusion MRI and tractography potentially provide novel biomarkers that connect volumetric changes across different brain regions. In a translation setting, these measurements constitute a novel tool to assess the therapeutic impact of interventions such as neuroprotective agents in transgenic models, as well as patients with Huntington's disease.

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Neuroimaging, Urinary, and Plasma Biomarkers of Treatment Response in Huntington's Disease: Preclinical Evidence with the p75NTR Ligand LM11A-31

Cited by 20 publications

References 135 publications

Clinical Correlates Identify ProBDNF and Thrombo-Inflammatory Markers as Key Predictors of Circulating p75NTR Extracellular Domain Levels in Older Adults

Clinical Correlates Identify ProBDNF and Thrombo-Inflammatory Markers as Key Predictors of Circulating p75NTR Extracellular Domain Levels in Older Adults

Current Diagnostic Methods and Non-Coding RNAs as Possible Biomarkers in Huntington’s Disease

Ex vivo 100 μm isotropic diffusion MRI‐based tractography of connectivity changes in the end‐stage R6/2 mouse model of Huntington's disease

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