Pharmacokinetics and pharmacodynamics of a single dose Nilotinib in individuals with Parkinson's disease

Pagán, Fernando; Hebron, Michaeline; Wilmarth, Barbara; Torres‐Yaghi, Yasar; Lawler, Abigail; Mundel, Elizabeth E.; Yusuf, Nadia; Starr, Nathan; Arellano, Joy; Howard, Helen H.; Peyton, Margo A; Matar, Sara; Liu, Xiaoguang; Fowler, Alan J.; Schwartz, Sorell L.; Ahn, Jaeil; Moussa, Charbel

doi:10.1002/prp2.470

Cited by 72 publications

(117 citation statements)

References 60 publications

(139 reference statements)

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“…9,11,[19][20][21] The single-dose study showed that changes of CSF dopamine metabolism with lower (150-200 mg) doses of nilotinib may be concurrent with a reduction of oligomeric α-synuclein in a time-dependent manner. 15 The CSF levels of α-synuclein oligomers increase in PD, while the total α-synuclein level decreases, compared with aged-matched controls. [22][23][24] There was no change of CSF total α-synuclein at 12 months, but the level of oligomeric α-synuclein was significantly reduced in the 150-mg, but not the 300-mg, nilotinib group.…”

Section: Research Original Investigationmentioning

confidence: 97%

“…At 12 months, the present study demonstrated an increase in CSF levels of dopamine metabolites in the nilotinib groups compared with the placebo group, which is consistent with previous results. 12,15 DOPAC is a principal metabolite of dopamine and the primary metabolite in humans. 17 Our data indicate an increase in CSF levels of HVA and CSF and plasma levels of DOPAC in the nilotinib 150-mg group.…”

Section: Research Original Investigationmentioning

confidence: 99%

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Nilotinib Effects on Safety, Tolerability, and Potential Biomarkers in Parkinson Disease

et al. 2020

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IMPORTANCE This study evaluated nilotinib safety and its effects on biomarkers as a potential disease-modifying drug in Parkinson disease.OBJECTIVES To assess nilotinib effects on safety and pharmacokinetics and measure the change in exploratory biomarkers in patients with moderately severe Parkinson disease. DESIGN, SETTING, AND PARTICIPANTSThis was a single-center, phase 2, randomized, double-blind, placebo-controlled trial with 300 patients approached in clinic; of these, 200 declined to participate, 100 were screened, 25 were excluded, and 75 were randomized 1:1:1 into placebo; nilotinib, 150-mg; or nilotinib, 300-mg groups. Recruitment started on May 17, 2017, and ended April 28, 2018, and follow-up ended August 10, 2019. Parkinson disease was confirmed according to the UK Brain Bank diagnostic criteria and symptoms were stabilized with use of optimal levodopa and/or dopamine agonists and other medications used in Parkinson disease.INTERVENTIONS Nilotinib vs placebo, administered orally once daily for 12 months followed by a 3-month washout period.MAIN OUTCOMES AND MEASURES It was hypothesized that nilotinib is safe and can be detected in the cerebrospinal fluid, where it alters exploratory biomarkers via inhibition of Abelson tyrosine kinase and potentially improves clinical outcomes. RESULTSOf the 75 patients included in the study, 55 were men (73.3%); mean (SD) age was 68.4 (8.2) years. Doses of 150 or 300 mg of nilotinib were reasonably safe, although more serious adverse events were detected in the nilotinib (150 mg: 6 [24%]; 300 mg: 12 [48%]) vs placebo (4 [16%]) groups. The 150-mg nilotinib group showed an increase in cerebrospinal fluid levels of the dopamine metabolites homovanillic acid (159.80nM; 90% CI, 7.04-312.60nM; P = .04) and 3,4-dihydroxyphenylacetic acid (4.87nM; 90% CI, 1.51-8.23nM; P = .01), and the 300-mg nilotinib group showed an increase in 3,4-dihydroxyphenylacetic acid (7.52nM; 90% CI, 2.35-12.69nM; P = .01). The nilotinib 150-mg but not the nilotinib 300-mg group demonstrated a reduction of α-synuclein oligomers (−0.04 pg/mL; 90% CI, −0.08 to 0.01 pg/mL; P = .03). A significant reduction of hyperphosphorylated tau levels was seen in the nilotinib 150-mg (−10.04 pg/mL; 90% CI, −17.41 to −2.67 pg/mL; P = .01) and nilotinib 300-mg (−12.05 pg/mL; 90% CI, −19.21 to −4.90 pg/mL; P = .01) groups.CONCLUSIONS AND RELEVANCE In this study, nilotinib appeared to be reasonably safe and detectable in the cerebrospinal fluid. Exploratory biomarkers were altered in response to nilotinib. Taken together, these data will guide the development of a phase 3 study to investigate the effects of nilotinib therapy in patients with Parkinson disease. TRIAL REGISTRATION ClinicalTrials.gov identifier: NCT02954978

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Section: Research Original Investigationmentioning

confidence: 97%

Section: Research Original Investigationmentioning

confidence: 99%

Nilotinib Effects on Safety, Tolerability, and Potential Biomarkers in Parkinson Disease

et al. 2020

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“…Some studies have also investigated the effects of Abelson tyrosine kinase (c‐Abl) inhibition on Beclin‐1‐mediated autophagic α‐syn clearance, throughout treatment with Nilotinib, which is usually used in patients with Philadelphia chromosome–positive chronic myelogenous leukemia . Nilotinib appeared to be potentially effective in treating motor and nonmotor symptoms in patients with PD and DLB . Currently, two trials investigating safety, pharmacokinetics, and pharmacodynamics of Nilotinib in patients affected by PD and PD with dementia (http://ClinicalTrials.gov ID:NCT02954978), as well as the ability of this molecule to pass the blood–brain barrier and to reach its target, are ongoing (http://ClinicalTrials.gov ID:NCT03205488).…”

Section: The Alp As a Possible Therapeutic Target For Pdmentioning

confidence: 99%

“…149,150 Nilotinib appeared to be potentially effective in treating motor and nonmotor symptoms in patients with PD and DLB. 151,152 Currently, two trials investigating safety, pharmacokinetics, and pharmacodynamics of Nilotinib in patients affected by PD and PD with dementia (ClinicalTrials.gov ID: NCT02954978), as well as the ability of this molecule to pass the blood-brain barrier and to reach its target, are ongoing (ClinicalTrials.gov ID:NCT03205488).…”

Section: The Alp As a Possible Therapeuticmentioning

confidence: 99%

The Vicious Cycle Between α‐Synuclein Aggregation and Autophagic‐Lysosomal Dysfunction

et al. 2019

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The accumulation and misfolding of α‐synuclein (α‐syn) represent the main pathological hallmark of PD. Overexpression of α‐syn and failure of cellular protein degradation systems play a major role in α‐syn aggregation. The discovery of PD‐associated genes related to the autophagic‐lysosomal pathway, such as VPS35, LRRK2, GBA1, SMPD1, GALC, ASAH1, SCARB2, CTSD, CTSB, and GLA, confirms the involvement of cellular clearance systems dysfunction in PD pathogenesis. Of importance, lysosomal enzyme activity is altered both in genetic and sporadic PD. Decreased lysosomal enzymes activities were measured in the same brain regions where α‐syn accumulates, suggesting that a crosstalk between α‐syn aggregation and autophagic‐lysosomal impairment may exist. The understanding of autophagic‐lysosomal pathway dysfunctions’ role in the pathogenesis and progression of synucleinopathies opened new perspectives for novel possible therapeutic strategies. In this article, the evidences and mechanisms of the reciprocal relation between autophagic‐lysosomal pathway impairment and misfolded α‐syn aggregation and propagation are reviewed, together with the most promising compounds targeting autophagic‐lysosomal pathway restoration as a disease‐modifying strategy for PD treatment. © 2019 International Parkinson and Movement Disorder Society

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“…Protein kinases represent central molecular hubs that regulate numerous cell processes, thus constituting potentially attractive clinical targets. Indeed, the success of kinase inhibitors in treating cancer has spurred the evaluation of such compounds in phase II/III clinical trials as candidates for treatment of various neurodegenerative diseases [22,23]. Since several kinases have been implicated in PD pathology [24], we screened a collection of 273 small molecule kinase inhibitors from Selleck Chemicals (Table S1) to identify molecules with prospective neuroprotective properties.…”

Section: High Content Screening Of a Kinase Inhibitor Library Identifmentioning

confidence: 99%

High Content Screening and Proteomic Analysis Identify a Kinase Inhibitor that rescues pathological phenotypes in a Patient-Derived Model of Parkinson’s Disease

Antoniou

Prodromidou

Kouroupi

et al. 2020

Preprint

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Combining high throughput screening approaches with induced pluripotent stem cell (iPSC)based disease models represents a promising unbiased strategy to identify therapies for neurodegenerative disorders. Here we applied high content imaging on iPSC-derived neurons from patients with familial Parkinson's disease bearing the G209A (p.A53T) α-synuclein (αSyn) mutation and launched a screening campaign on a small kinase inhibitor library. We thus identified the multi-kinase inhibitor BX795 that at a single dose effectively restores diseaseassociated neurodegenerative phenotypes. Proteomics profiling mapped the molecular pathways underlying the neuroprotective effects of BX795 that comprised a cohort of 118 protein-mediators of the core biological processes of RNA metabolism, protein synthesis, modification and clearance, and stress response, all linked to the mTORC1 signaling hub. In agreement, expression of human p.A53T-αSyn in neuron-like cells affected key components of the mTORC1 pathway resulting in aberrant protein synthesis that was restored in the presence of BX795 with concurrent facilitation of autophagy. Taken together, we have developed an adaptable platform based on p.A53T iPSC-derived neurons for drug screening and identified a promising small molecule with potent neuroprotective actions as candidate therapeutic for PD and other protein conformational disorders.3 Key words α-synuclein, p.A53T α-synuclein mutation, induced pluripotent stem cell derived neurons, drug screening, mTOR signaling, mRNA metabolism, proteostasis AcknowledgementsWe thank Drs. Tamotsu Yoshimori and Terje Johansen for providing GFP-LC3 and mChery-GFP-p62 plasmids, respectively.

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Pharmacokinetics and pharmacodynamics of a single dose Nilotinib in individuals with Parkinson's disease

Cited by 72 publications

References 60 publications

Nilotinib Effects on Safety, Tolerability, and Potential Biomarkers in Parkinson Disease

Nilotinib Effects on Safety, Tolerability, and Potential Biomarkers in Parkinson Disease

The Vicious Cycle Between α‐Synuclein Aggregation and Autophagic‐Lysosomal Dysfunction

High Content Screening and Proteomic Analysis Identify a Kinase Inhibitor that rescues pathological phenotypes in a Patient-Derived Model of Parkinson’s Disease

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