遗传朊病毒病风险个体在疾病转化前的体液生物标志物。

Fluid Biomarkers in Individuals at Risk for Genetic Prion Disease up to Disease Conversion.

机构信息

From the McCance Center for Brain Health (S.M.V., M.A.M., E.V.M.) and Department of Neurology (S.M.V., M.A.M., S.W.A., A.C.K., P.K., B.L.H., A.B., B.A.T., K.D.-M., A.M.F., L.E.S., G.D., A.R., J.G., A.J.M., E.V.M., S.E.A.), Massachusetts General Hospital, Boston; Stanley Center for Psychiatric Research (S.M.V., M.A.M., E.V.M.), Broad Institute of MIT and Harvard, Cambridge; and Department of Neurology (S.M.V., P.K., E.V.M., S.E.A.), Harvard Medical School, Boston, MA.

出版信息

Neurology. 2024 Jul 23;103(2):e209506. doi: 10.1212/WNL.0000000000209506. Epub 2024 Jun 19.

DOI:10.1212/WNL.0000000000209506

PMID:38896810

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11226308/

Abstract

OBJECTIVES

To longitudinally characterize disease-relevant CSF and plasma biomarkers in individuals at risk for genetic prion disease up to disease conversion.

METHODS

This single-center longitudinal cohort study has followed known carriers of pathogenic variants at risk for prion disease, individuals with a close relative who died of genetic prion disease but who have not undergone predictive genetic testing, and controls. All participants were asymptomatic at first visit and returned roughly annually. We determined genotypes, measured NfL and GFAP in plasma, and RT-QuIC, total PrP, NfL, T-tau, and beta-synuclein in CSF.

RESULTS

Among 41 carriers and 21 controls enrolled, 28 (68%) and 15 (71%) were female, and mean ages were 47.5 and 46.1. At baseline, all individuals were asymptomatic. We observed RT-QuIC seeding activity in the CSF of 3 asymptomatic E200K carriers who subsequently converted to symptomatic and died of prion disease. 1 P102L carrier remained RT-QuIC negative through symptom conversion. No other individuals developed symptoms. The prodromal window from detection of RT-QuIC positivity to disease onset was 1 year long in an E200K individual homozygous (V/V) at PRNP codon 129 and 2.5 and 3.1 years in 2 codon 129 heterozygotes (M/V). Changes in neurodegenerative and neuroinflammatory markers were variably observed prior to onset, with increases observed for plasma NfL in 4/4 converters, and plasma GFAP, CSF NfL, CSF T-tau, and CSF beta-synuclein each in 2/4 converters, although values relative to age and fold changes relative to individual baseline were not remarkable for any of these markers. CSF PrP was longitudinally stable with mean coefficient of variation 9.0% across all individuals over up to 6 years, including data from converting individuals at RT-QuIC-positive timepoints.

DISCUSSION

CSF prion seeding activity may represent the earliest detectable prodromal sign in E200K carriers. Neuronal damage and neuroinflammation markers show limited sensitivity in the prodromal phase. CSF PrP levels remain stable even in the presence of RT-QuIC seeding activity.

CLINICAL TRIALS REGISTRATION

ClinicalTrials.gov NCT05124392 posted 2017-12-01, updated 2023-01-27.

摘要

目的

对遗传朊病毒病风险个体的脑脊液（CSF）和血浆生物标志物进行纵向特征分析，直至疾病转化。

方法

本单中心纵向队列研究对朊病毒病致病性变异的已知携带者、有近亲死于遗传朊病毒病但未接受预测性基因检测的个体以及对照组进行了随访。所有参与者在首次就诊时均无症状，并大致每年返回一次。我们确定了基因型，测量了血浆中的 NfL 和 GFAP，并检测了 CSF 中的 RT-QuIC、总 PrP、NfL、T-tau 和 beta-突触核蛋白。

结果

在纳入的 41 名携带者和 21 名对照者中，28 名（68%）和 15 名（71%）为女性，平均年龄分别为 47.5 岁和 46.1 岁。基线时，所有个体均无症状。我们观察到 3 名无症状 E200K 携带者的 CSF 中存在 RT-QuIC 种籽活性，随后这些携带者发展为有症状并死于朊病毒病。1 名 P102L 携带者在症状转换时仍为 RT-QuIC 阴性。其他个体均未出现症状。在 PRNP 密码子 129 处纯合（V/V）的 E200K 个体中，从 RT-QuIC 阳性检测到疾病发作的前驱期窗口长达 1 年，而在 2 名密码子 129 杂合子（M/V）中分别为 2.5 年和 3.1 年。在发病前，神经退行性和神经炎症标志物的变化是可变的，4/4 名转化者的血浆 NfL 增加，2/4 名转化者的血浆 GFAP、CSF NfL、CSF T-tau 和 CSF beta-突触核蛋白增加，尽管这些标志物的年龄相关值和个体基线的倍数变化均不显著。CSF PrP 在长达 6 年的时间内保持稳定，所有个体的平均变异系数为 9.0%，包括 RT-QuIC 阳性时间点的转化个体的数据。

讨论

CSF 朊病毒种籽活性可能代表 E200K 携带者最早可检测到的前驱期征象。在前驱期，神经元损伤和神经炎症标志物的敏感性有限。即使存在 RT-QuIC 种籽活性，CSF PrP 水平仍保持稳定。

临床试验注册

ClinicalTrials.gov NCT05124392 于 2017 年 12 月 1 日注册，2023 年 1 月 27 日更新。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7687/11226308/ababf249daf9/WNL-2024-100338f1.jpg

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遗传朊病毒病风险个体在疾病转化前的体液生物标志物。

Fluid Biomarkers in Individuals at Risk for Genetic Prion Disease up to Disease Conversion.

机构信息

出版信息

Neurology. 2024 Jul 23;103(2):e209506. doi: 10.1212/WNL.0000000000209506. Epub 2024 Jun 19.

DOI:10.1212/WNL.0000000000209506

PMID:38896810

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11226308/

Abstract

OBJECTIVES

To longitudinally characterize disease-relevant CSF and plasma biomarkers in individuals at risk for genetic prion disease up to disease conversion.

METHODS

RESULTS

DISCUSSION

CLINICAL TRIALS REGISTRATION

ClinicalTrials.gov NCT05124392 posted 2017-12-01, updated 2023-01-27.

摘要

目的

对遗传朊病毒病风险个体的脑脊液（CSF）和血浆生物标志物进行纵向特征分析，直至疾病转化。

方法

结果

讨论

临床试验注册

ClinicalTrials.gov NCT05124392 于 2017 年 12 月 1 日注册，2023 年 1 月 27 日更新。

遗传朊病毒病风险个体在疾病转化前的体液生物标志物。

Fluid Biomarkers in Individuals at Risk for Genetic Prion Disease up to Disease Conversion.

机构信息

出版信息

OBJECTIVES

METHODS

RESULTS

DISCUSSION

CLINICAL TRIALS REGISTRATION

目的

方法

结果

讨论

临床试验注册

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遗传朊病毒病风险个体在疾病转化前的体液生物标志物。

Fluid Biomarkers in Individuals at Risk for Genetic Prion Disease up to Disease Conversion.

机构信息

出版信息

OBJECTIVES

METHODS

RESULTS

DISCUSSION

CLINICAL TRIALS REGISTRATION

目的

方法

结果

讨论

临床试验注册