NCT03687476

Brief Summary

This is a Phase-2, multicenter, multiple dose, open-label, 2-part evaluation study which will primarily assess the safety and tolerability of VTS-270 (2-hydroxypropyl beta-cyclodextrin \[HP-β-CD\]) in pediatric participants with age \<4 years.

Trial Health

15
At Risk

Trial Health Score

Automated assessment based on enrollment pace, timeline, and geographic reach

Trial has exceeded expected completion date
Timeline
Completed

Started May 2020

Status
withdrawn

Health score is calculated from publicly available data and should be used for screening purposes only.

Trial Relationships

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Study Timeline

Key milestones and dates

First Submitted

Initial submission to the registry

August 6, 2018

Completed
2 months until next milestone

First Posted

Study publicly available on registry

September 27, 2018

Completed
1.6 years until next milestone

Study Start

First participant enrolled

May 1, 2020

Completed
2.5 years until next milestone

Primary Completion

Last participant's last visit for primary outcome

October 30, 2022

Completed
Same day until next milestone

Study Completion

Last participant's last visit for all outcomes

October 30, 2022

Completed
Last Updated

July 22, 2020

Status Verified

July 1, 2020

Enrollment Period

2.5 years

First QC Date

August 6, 2018

Last Update Submit

July 20, 2020

Conditions

Niemann-Pick Disease, Type C

Outcome Measures

Primary Outcomes (5)

  • Number of Participants With Treatment-Emergent Adverse Events (AEs) or Serious Adverse Events (SAEs): Part A

    An AE is any untoward medical occurrence in a participant who received study drug without regard to possibility of causal relationship. An SAE is an AE resulting in any of the following outcomes or deemed significant for any other reason: death; initial or prolonged inpatient hospitalization; life-threatening experience (immediate risk of dying); persistent or significant disability/incapacity; congenital anomaly. Treatment-emergent are events between first dose of study drug and up to 28 days after last dose that were absent before treatment or that worsened relative to pre-treatment state. SAEs were AEs excluding non-serious AEs.

    Baseline up to Week 20 (End of Part A)

  • Number of Participants With Clinically Significant Vital Signs: Part A

    Clinically significant vital sign is defined as an abnormal vital sign result that results in a treatment-emergent AEs. Abnormal clinically significant vital signs included absolute systolic blood pressure (BP) values less than (\<) 90 millimeter of mercury (mmHg), maximum increase or decrease of greater than or equal to (\>=) 30 mmHg from baseline for systolic BP; absolute diastolic BP \<50 mmHg with maximum increase or decrease of \>=20 mmHg from baseline and absolute heart rate values \<40 beats per minute (bpm), \>120 bpm for supine or sitting measurement, \>140 bpm for standing measurement, temperature \<32 or \>40 degree centigrade, respiratory rate of \<10 or \>50 breaths/minute.

    Baseline up to Week 20 (End of Part A)

  • Number of Participants With Clinically Significant Change from Baseline in Body Weight: Part A

    Any change from baseline in body weight is considered by the investigator to be clinically significant and will be recorded as treatment-emergent AE.

    Baseline up to Week 20 (End of Part A)

  • Number of Participants With Clinically Significant Change from Baseline in Body Height: Part A

    Any change from baseline in body height is considered by the investigator to be clinically significant and will be recorded as treatment-emergent AE.

    Baseline up to Week 20 (End of Part A)

  • Number of Participants With Clinically Significant Laboratory Test Abnormalities: Part A

    Criteria for laboratory tests abnormalities included: hemoglobin, hematocrit and red blood cells (\< 0.8\*lower limit of normal\[LLN\]); leucocytes (\<0.6/\>1.5\*upper limit of normal \[ULN\]); platelets (\<0.5\*LLN/\>1.75\*ULN); neutrophils, lymphocytes (\<0.8\*LLN/\>1.2\*ULN); eosinophils, basophils, monocytes (\>1.2\*ULN); total bilirubin (\>1.5\*ULN); aspartate aminotransferase (AST), alanine aminotransferase (ALT), alkaline phosphatase (\>3\*ULN), total protein, albumin (\<0.8\*LLN/\>1.2\*ULN); creatinine, urea (\>1.3\*ULN); glucose (\<0.6\*LLN/\>1.5\*ULN); uric acid (\>1.2\*ULN); sodium, potassium, chloride, calcium, bicarbonate (\<0.9\*LLN/\>1.1\*ULN); urine red blood cells (RBCs), urine white blood cells (WBCs), urine epithelial cells (\>=6 high-powered field), urine bacteria \>20 high-powered field; qualitative urine glucose, ketones, protein values \>=1 in urine dipstick test. Total number of participants with any laboratory abnormalities was reported.

    Baseline up to Week 20 (End of Part A)

Secondary Outcomes (10)

  • Number of Participants With Treatment-Emergent Adverse Events (AEs) or Serious Adverse Events (SAEs): Part B

    Week 22 up to 3 years (End of Study or Part B)

  • Number of Participants With Clinically Significant Vital Signs: Part B

    Week 22 up to 3 years (End of Study or Part B)

  • Number of Participants With Clinically Significant Change from Baseline in Body Weight: Part B

    Week 22 up to 3 years (End of Study or Part B)

  • Number of Participants With Clinically Significant Change from Baseline in Body Height: Part B

    Week 22 up to 3 years (End of Study or Part B)

  • Number of Participants With Clinically Significant Laboratory Test Abnormalities: Part B

    Week 22 up to 3 years (End of Study or Part B)

  • +5 more secondary outcomes

Study Arms (2)

VTS-270 (Part A)

EXPERIMENTAL

VTS-270 200 milligram per milliliter (mg/mL) will be administered intrathecally by lumbar puncture every 2 weeks followed by dose escalation of 100 mg/mL increments up to a maximum tolerable dose of 900 mg/mL. The highest tolerable dose is considered as clinically relevant dose which will be administered throughout the remaining duration of the 20-week treatment period of Part A.

Drug: VTS-270

VTS-270 (Part B)

EXPERIMENTAL

VTS-270 200 mg/mL will be administered intrathecally by lumbar puncture every 2 weeks in Part B followed by a re-challenge to dose escalation of 100 mg/mL increments up to a maximum tolerable dose of 900 mg/mL. In case of intolerance, the dose should be returned to previously tolerable dose and should be continued throughout the duration of Part B (end of study).

Drug: VTS-270

Interventions

VTS-270DRUG

VTS-270 200 mg/mL administered as described in the arm group description.

VTS-270 (Part A)VTS-270 (Part B)

Eligibility Criteria

AgeUp to 4 Years
Sexall
Healthy VolunteersNo
Age GroupsChild (0-17)

You may qualify if:

  • The parent(s)/legal guardian(s) must be adequately informed and understand the nature and risks of the study. The participant's parent or legal guardian must provide a signature and date on the informed consent form (ICF).
  • Participants must have neurologial symptoms defined as, any area of developmental delay 1 SD below the mean (example, developmental quotient or standard score under 85 in any domain on the Mullen Scale Early Learning \[MSEL\]) or a significant developmental quotient /standard score drop on the MSEL.
  • Diagnosis of NPC determined by one of the following:
  • Two NPC1 or NPC2 mutations;
  • Positive filipin staining or oxysterol testing and at least one NPC1 or NPC2 mutation;
  • Vertical supranuclear gaze palsy in combination with either:
  • i. One NPC1/NPC2 mutation, or
  • ii. Positive filipin staining or oxysterol levels consistent with NPC1 or NPC2 disease.
  • If taking miglustat (Zavesca), participant(s) must have been on a stable dose for 6 weeks prior to the Screening Visit and willing to remain on a stable dose for the duration of participation in this study. If not taking migulstat, the participant must have been off treatment for a minimum of 6 weeks prior to the Baseline Visit.
  • If a participant has a history of seizures, the condition must be adequately controlled (the pattern of seizure activity must be stable) and the participant must be on a stable dose and regimen of antiepileptic medication(s) 4 weeks prior to the Screening Visit.
  • Prior exposure to VTS-270 is permitted.
  • The participant's parent(s)/legal guardian(s) are able to communicate effectively with study personnel.
  • Parent(s)/legal guardian(s) are able and willing to follow all protocol requirements and study restrictions.
  • Parent(s)/legal guardian(s) are able and willing to return participants for all study visits.

You may not qualify if:

  • Is from a vulnerable population, as defined by the US CFR Title 45, Part 46, Section 46.111(b) and other local and national regulations, including but not limited to, employees (temporary, part-time, full time, etc) or a family member of the research staff conducting the study, or of the sponsor, or of the contract research organization, or of the institutional review board (IRB)/independent ethics committee (IEC).
  • Has a history of sensitivity or allergy to any product containing HP-β-CD.
  • A history of hypersensitivity reactions or allergy to the anesthetic and/or sedative agents to be used for the lumbar puncture procedure.
  • Taken an anticoagulant in the 2 weeks prior to the Baseline Visit or plan to use anticoagulants during the study.
  • Change in antiepileptic treatment between the Screening Visit and the Baseline Visit.
  • Received treatment for any investigational product (exclusive of VTS-270) within 4 weeks of the Baseline Visit or at least 5 half-lives, whichever criteria is longest.
  • A suspected infection of the central nervous system or any systemic infection.
  • A spinal deformity that is likely to impact the ability to perform repeated LPs.
  • Evidence of obstructive hydrocephalus or normal pressure hydrocephalus.
  • A known bleeding disorder.
  • Has any of the following laboratory abnormalities ( greater than 1.5 times the upper limit of normal) at the Screening Visit:
  • Neutropenia
  • Thrombocytopenia
  • Activated partial thromboplastin time
  • Prothrombin time prolongation.
  • +3 more criteria

Contact the study team to confirm eligibility.

Sponsors & Collaborators

MeSH Terms

Conditions

Niemann-Pick Disease, Type C

Condition Hierarchy (Ancestors)

Niemann-Pick DiseasesSphingolipidosesLysosomal Storage Diseases, Nervous SystemBrain Diseases, Metabolic, InbornBrain Diseases, MetabolicBrain DiseasesCentral Nervous System DiseasesNervous System DiseasesHistiocytosis, Non-Langerhans-CellHistiocytosisLymphatic DiseasesHemic and Lymphatic DiseasesMetabolism, Inborn ErrorsGenetic Diseases, InbornCongenital, Hereditary, and Neonatal Diseases and AbnormalitiesLipidosesLipid Metabolism, Inborn ErrorsLysosomal Storage DiseasesMetabolic DiseasesNutritional and Metabolic DiseasesLipid Metabolism Disorders

Study Officials

  • Global Clinical Leader

    Mallinckrodt

    STUDY DIRECTOR
0

Study Design

Study Type
interventional
Phase
phase 2
Allocation
NON RANDOMIZED
Masking
NONE
Purpose
TREATMENT
Intervention Model
SEQUENTIAL
Sponsor Type
INDUSTRY
Responsible Party
SPONSOR

Study Record Dates

First Submitted

August 6, 2018

First Posted

September 27, 2018

Study Start

May 1, 2020

Primary Completion

October 30, 2022

Study Completion

October 30, 2022

Last Updated

July 22, 2020

Record last verified: 2020-07

Data Sharing

IPD Sharing
Will not share