Diagnostic Potential of Neural Exosome Cargo as Biomarkers for Acute Brain Injury

Goetzl, Laura; Merabova, Nana; Darbinian, Nune; Martirosyan, Diana; Poletto, Erica; Fugarolas, Keri; Menkiti, Ogechukwu

doi:10.1002/acn3.499

Cited by 52 publications

(46 citation statements)

References 38 publications

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“…Some progress has been made in the study of exosomes as biomarkers for neurological diseases. Neural exosomes are diagnostic biomarkers for acute brain injury (Goetzl et al, 2017). Serum exosome SNAP-25 is a potential biomarker of Alzheimer's disease (Agliardi et al, 2019).…”

Section: Discussionmentioning

confidence: 99%

Serum Exosomal Proteins F9 and TSP-1 as Potential Diagnostic Biomarkers for Newly Diagnosed Epilepsy

Lin

Zhou

et al. 2020

Front. Neurosci.

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Epilepsy is one of the most common chronic neurological diseases in the world, with a high incidence, a high risk of sudden unexplained death, and diagnostic challenges. Exosomes are nanosized extracellular vesicles that are released into physical environments and carry a variety of biological information. Moreover, exosomes can also be synthesized and released from brain cells, passing through the blood-brain barrier, and can be detected in peripheral blood or cerebrospinal fluid. Our study using the tandem mass tag (TMT) approach showed that a total of 76 proteins were differentially expressed in serum exosomes between epilepsy patients and healthy controls, with 6 proteins increasing and 70 proteins decreasing. Analysis of large clinical samples and two mouse models of chronic epilepsy indicated that two significantly differentially expressed serum exosomal proteins, coagulation factor IX (F9) and thrombospondin-1 (TSP-1), represent promising biomarkers for the diagnosis of epilepsy, with area under the curve (AUC) values of up to 0.7776 (95% CI, 0.7306-0.8246) and 0.8534 (95% CI, 0.8152-0.8916), respectively. This is the first study of exosomal proteins in epilepsy, and it suggests that exosomes are promising new tools for the diagnosis of epilepsy.

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Section: Discussionmentioning

confidence: 99%

Serum Exosomal Proteins F9 and TSP-1 as Potential Diagnostic Biomarkers for Newly Diagnosed Epilepsy

Lin

Zhou

et al. 2020

Front. Neurosci.

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“…), synaptopodin (BioMatik‐EKU07541, Wilmington, DE), and neurogranin (American Research Products/CEA404HU, Waltham, MA) were also quantified by ELISA. These proteins were chosen as we had previously validated them as CNS exosome markers, including in a study of hypoxic injury in neonates . The mean value for all determinations of CD81 in each assay group was set at 1.00 and the relative values for each sample used to normalize their recovery.…”

Section: Methodsmentioning

confidence: 99%

“…Fresh placenta tissue was immediately rinsed in cold phosphate‐buffered saline (PBS) to remove any blood or decidua. Apical brush border membrane fractions were prepared according to published protocols and solubilized in lysis buffer (50mM Tris‐HCl, pH 7.4, 150mM NaCl, 0.1 % Nonidet P‐40, and 1% protease inhibitors cocktail, Sigma). Samples were homogenized in ice, placed in wash buffer with MgCl2 (10mM final concentration), stir for 3 minutes and then incubate on ice for 10 minutes.…”

Section: Methodsmentioning

confidence: 99%

Noninvasive assessment of fetal central nervous system insult: Potential application to prenatal diagnosis

2019

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Objective: We have developed novel methods for isolating fetal central nervous system (CNS)-derived extracellular vesicles (FCEs) from maternal plasma as a noninvasive platform for testing aspects of fetal neurodevelopment in early pregnancy.We investigate the hypothesis that levels of defined sets of functional proteins in FCEs can be used to detect abnormalities in fetal neuronal and glial proliferation, differentiation, and survival.Method: Maternal plasma was obtained between 10 and 19 weeks from women with current heavy EtOH exposure and matched controls. FCE levels of synaptophysin, synaptotagmin, synaptopodin, and neurogranin were quantified normalized to the exosome marker CD81. Quantitative RT-PCR was performed with specific primers for miR-9.Results: FCE cargo protein levels of synaptophysin, synaptotagmin, synaptopodin, and neurogranin were all significantly reduced in pregnancies exposed to current heavy EtOH use (P < .001 for all). Both synaptophysin and neurogranin appeared to be particularly discriminatory with no overlap between exposed and control subjects.Up to tenfold inhibition (90%) in MicroRNA-9 was observed in FCEs from EtOH exposed fetuses compared with controls. Conclusion:Our results suggest that FCEs purified from maternal plasma may be a powerful tool to assess abnormal proliferation and differentiation of CNS stem cells as early as the late first trimester.

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“…Between 47% and 81% of newborns with gestational methadone or buprenorphine exposure will require pharmacotherapy. 22,23 Thus FCEs could be a new tool to interrogate in vivo neurodevelopment involving elements of opioid signaling pathways, including proteins (mu-opioid receptor [μOR], cannabinoid receptors) and microRNAs (miRNAs). 20,21 None of these factors are sufficient to reliably predict NAS severity, and the mechanisms by which they impact NAS are not well understood.…”

Section: Introductionmentioning

confidence: 99%

“…22 Our published findings show that purified FCEs can be used to detect fetal CNS damage caused by in utero alcohol exposure, hypoxia and viral infection. 22,23 Thus FCEs could be a new tool to interrogate in vivo neurodevelopment involving elements of opioid signaling pathways, including proteins (mu-opioid receptor [μOR], cannabinoid receptors) and microRNAs (miRNAs). miRNAs are a class of small (17 to 24 nucleotides) noncoding RNAs that target the untranslated region of messenger RNAs to silence genes posttranscriptionally.…”

Section: Introductionmentioning

confidence: 99%

Novel biomarkers to assess in utero effects of maternal opioid use: First steps toward understanding short‐ and long‐term neurodevelopmental sequelae

Goetzl

Thompson-Felix

Darbinian

et al. 2019

Genes Brain and Behavior

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Maternal opioid use disorder is common, resulting in significant neonatal morbidity and cost. Currently, it is not possible to predict which opioid‐exposed newborns will require pharmacotherapy for neonatal abstinence syndrome. Further, little is known regarding the effects of maternal opioid use disorder on the developing human brain. We hypothesized that novel methodologies utilizing fetal central nervous system‐derived extracellular vesicles isolated from maternal blood can address these gaps in knowledge. Plasma from opioid users and controls between 9 and 21 weeks was precipitated and extracellular vesicles were isolated. Mu opioid and cannabinoid receptor levels were quantified. Label‐free proteomics studies and unbiased small RNA next generation sequencing was performed in paired fetal brain tissue. Maternal opioid use disorder increased mu opioid receptor protein levels in extracellular vesicles independent of opioid equivalent dose. Moreover, cannabinoid receptor levels in extracellular vesicles were upregulated with opioid exposure indicating cross talk with endocannabinoids. Maternal opioid use disorder was associated with significant changes in extracellular vesicle protein cargo and fetal brain micro RNA expression, especially in male fetuses. Many of the altered cargo molecules and micro RNAs identified are associated with adverse clinical neurodevelopmental outcomes. Our data suggest that assays relying on extracellular vesicles isolated from maternal blood extracellular vesicles may provide information regarding fetal response to opioids in the setting of maternal opioid use disorder. Prospective clinical studies are needed to evaluate the association between extracellular vesicle biomarkers, risk of neonatal abstinence syndrome and neurodevelopmental outcomes.

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Diagnostic Potential of Neural Exosome Cargo as Biomarkers for Acute Brain Injury

Cited by 52 publications

References 38 publications

Serum Exosomal Proteins F9 and TSP-1 as Potential Diagnostic Biomarkers for Newly Diagnosed Epilepsy

Serum Exosomal Proteins F9 and TSP-1 as Potential Diagnostic Biomarkers for Newly Diagnosed Epilepsy

Noninvasive assessment of fetal central nervous system insult: Potential application to prenatal diagnosis

Novel biomarkers to assess in utero effects of maternal opioid use: First steps toward understanding short‐ and long‐term neurodevelopmental sequelae

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