TP10 Use in Patients With C3 Glomerulopathy (C3G)
| Status: | Recruiting |
|---|---|
| Healthy: | No |
| Age Range: | 4 - Any |
| Updated: | 4/2/2016 |
| Start Date: | November 2014 |
| End Date: | December 2016 |
| Contact: | Richard JH Smith, MD |
| Email: | richard-smith@uiowa.edu |
| Phone: | 319-356-2177 |
A Pilot, Open-Label Single Center Trial of TP10 in Pediatric and Adult Patients With C3 Glomerulopathy (C3G)
The purpose of this study is to evaluate the safety of repeated TP10 dosing in pediatric and
adult patients with C3G and to evaluate the activity of TP10 in pediatric and adult patients
with C3G, as measured by the proportion of patients with normalization of serum C3, serum C3
breakdown products, or alternative pathway (AP) complement activity.
adult patients with C3G and to evaluate the activity of TP10 in pediatric and adult patients
with C3G, as measured by the proportion of patients with normalization of serum C3, serum C3
breakdown products, or alternative pathway (AP) complement activity.
Overview of Study Design: This study is a pilot Phase I, open-label, non-randomized,
single-arm, clinical trial of TP10 in 5 patients with C3G, aged 4 years or older. The study
consists of a 4-week screening period followed by a 26-week treatment period. (See Schedule
of Events, Table 1.) The 26-week treatment period is further divided into an Induction
Period of up to 4 weeks, followed by a Maintenance Period, which allows for continued
treatment to a total of 26 weeks.
Screening Period: Patients will be identified for possible enrollment in this study through
a number of mechanisms, including physician or patient-self referral and participation in an
on-going study of C3G in which renal pathology is reviewed to confirm the diagnosis of C3G
and genetic and complement studies are performed. Patients who appear to meet eligibility
criteria for this study upon initial review will be asked to contact Drs. Nester and Smith
if they are interested in this study. Those patients who express interest in this study will
be scheduled for a screening clinic visit at which time they will meet the study team and
review the study design and requirements. A consent for study participation will be
obtained. During this visit those events/tests noted on Table 1, Screening Visit, will be
completed. If not already vaccinated within the time period of active coverage specified by
the vaccine manufacturer, patients will be administered meningococcal, pneumococcal and
haemophilus influenzae vaccines prior to study drug administration.
Treatment Period: All patients will be enrolled through the University of Iowa. This study
will follow a patient-specific dose-escalation scheme during the Induction Period and
subsequent dose adjustments based on complement levels during the Maintenance Period (as
described under Investigational Product Dosing and Administration).
Safety Monitoring: Safety data for this trial will be reviewed by a Data Monitoring and
Safety Person (DMSP) consisting of one reviewer who is otherwise independent of trial
conduct, as well as study investigators. The DMSP will review safety data on a periodic
basis based on the accrual rate and emergence of safety data. The DMSP will evaluate patient
data with the purpose of identifying safety concerns that may require a modification of the
current study protocol and will also be responsible for determining if criteria for halting
of the trial are met (see below).
Study Stopping Rules: If any of the following criteria are met, further enrollment into the
trial will be halted and the data reviewed with the DMSP. The trial will only be reopened
after a mutually agreed plan is defined with the DMSP.
- Futility in the first three patients. Futility is defined as:
- Failure during the Induction Period to normalize C3, C3 breakdown products or
alternative pathway complement activity
- Any of the following toxicities in more than one patient:
- Dose-limiting toxicity (DLT), defined as any Grade 3 or higher drug-related
adverse event (AE)
- Grade 3 or higher infection caused by encapsulated bacteria, not responsive to
appropriate medical intervention within 24 hours
- Drug-related death Investigational Product Dosing and Administration Each TP10
administration will consist of a 60 (±5)-minute intravenous drip infusion using a 0.22
µm in-line filter and a controlled-rate infusion pump. Administered doses will range
from 5 mg/kg to 30 mg/kg, as determined by patient-specific dose-escalation and
adjustment. Any change in weight of more than 10% will require re-calculation of the
administered dose; otherwise, dosing may be based on the baseline weight. All dosing
will be bi-weekly during induction and weekly during maintenance.
To determine the effect of TP10 on complement and C3 convertase inhibition, complement
studies will include measuring TP10 serum concentrations and serum levels of C3 and C3
breakdown products and assays of alternative pathway function. Testing will be done on serum
and plasma samples obtained prior to and approximately 15 minutes post each TP10 dose. All
complement studies will be performed at the University of Iowa. The following treatment plan
will be followed for each patient. However, given the limited experience with TP10 in the
treatment of C3G, as well as the breadth of complement studies that may be used to assess
the impact of treatment, it is acknowledged that the treatment plan within this pilot study
may not account for all potential clinical scenarios. Therefore, adjustments to dose level
or frequency that fall outside of this plan may be implemented when determined clinically
appropriate by the lead investigators at the University of Iowa. In such cases, the IRB will
be notified of the plan for dose change.
Induction Period During the Induction Period, samples for complement studies will be
analyzed at least weekly. The first two doses of the Induction Period will be 5 mg/kg.
Intra-patient dose-escalation will subsequently occur weekly, in 5 or 10 mg/kg increments
(as determined by the investigator, based on complement biomarker changes), up to a maximum
dose of 30 mg/kg.
The Induction Period schedule will be modified when either of the following criteria are
met:
- Dose escalation will discontinue when normalization of C3, C3 breakdown products AND/OR
measure(s) of alternative and/or terminal pathway complement activity is achieved.
Thereafter, the patient will receive one additional TP10 dose at the same dose level as
the prior dose, and then transition to the Maintenance Period.
- If the dose level of 30 mg/kg is reached without normalization of C3, C3 breakdown
products AND/OR measure(s) of alternative and/or terminal pathway complement activity,
the patient may receive one additional dose of TP10 at 30 mg/kg.
- If normalization of C3, C3 breakdown products AND/OR measure(s) of alternative
and/or terminal pathway complement activity fails to occur, treatment will be
discontinued.
- If normalization of C3, C3 breakdown products AND/OR measure(s) of alternative
and/or terminal pathway complement activity occurs, the patient will enter the
Maintenance Period and follow rules for Maintenance Period dose adjustments.
In addition, study drug dosing will be discontinued if any additional criteria for
discontinuation of study therapy (see below) are met.
Maintenance Period
Since it is quite possible that the dose required for maintenance may be significantly lower
than that required during induction, the Maintenance Period will seek to identify the lowest
dose that provides ongoing control of undesirable complement activity. The starting dose for
TP10 Maintenance will be the same dose level as the last dose during the Induction Period;
however, the Maintenance Period allows for dose decrease to 2 mg/kg, which is lower than the
starting dose in the Induction Period. Samples for complement studies will be collected on
each dosing day and analyzed at least weekly at University of Iowa during the Maintenance
Period. Therefore, treatment decisions will be made at least weekly, and dose adjustments
throughout the Maintenance period will be implemented as follows (see Section 8.3.2 for
further details):
- If C3, C3 breakdown products AND/OR measure(s) of alternative and/or terminal pathway
complement activity are normalized for two consecutive weeks, the next Maintenance dose
may be decreased by 5 mg/kg (if the previous dose is 5 mg/kg, dosing will decrease to 2
mg/kg).
o Note: The dose level MAY be maintained if deemed appropriate by the treating
investigator, with consideration to factors such as biomarker evidence of neo-C3
convertase generation and overall profile of labs utilized for defining maintenance.
- If C3 levels have dropped >25% compared to entry into the Maintenance Period, C3
breakdown products are present (greater than normal), AND/OR measure(s) of alternative
or terminal pathway complement activity have significantly changed (>50% worsening in
value), the next Maintenance dose will be increased by 5 mg/kg up to a maximum of 30
mg/kg (if the previous dose is 2 mg/kg, dosing will increase to 5 mg/kg).
- If a patient has experienced dose reduction and subsequent dose escalation twice,
further dose reductions may not be required, but can be implemented at the
investigator's discretion. Otherwise, these patients may be maintained at the last dose
that provided normalization of C3, C3 breakdown products AND/OR alternative and/or
terminal pathway complement activity unless there are changes requiring a dose
increased, as described above.
- If normalization of C3, C3 breakdown products AND/OR alternative and/or terminal
pathway complement activity fails to occur despite receipt of 30 mg/kg twice weekly
dosing for two weeks, the patient will be withdrawn from the study.
The Maintenance Period will be continued until either:
- The total study treatment period of 26 weeks has elapsed;
- Any additional criteria for discontinuation of study therapy (see below) are met.
Additional criteria for treatment discontinuation
At any point during the study, treatment will be discontinued for any of the following
reasons:
- Decrease in renal function, defined by an increase in serum creatinine by 50% over
baseline (last assessment prior to first TP10 dose), persistent for 4 weeks.
- Development of dose-limiting toxicity (DLT), defined as any Grade 3 or higher AE
attributed to TP10 dosing, or any Grade 3 infection caused by encapsulated bacteria,
not responsive to appropriate medical intervention within 24 hours. Patients who
experience DLT but who are considered by the treating investigator to be potentially
appropriate for further TP10 treatment may be retreated only after consultation with,
and agreement from, the DMSP.
- The study is terminated (see early stopping rules).
- Request of the patient or the patient's legal representative.
- If, in the investigator's medical judgment, further participation would be injurious to
the patient's health or wellbeing.
- Non-compliance of the patient.
- Pregnancy.
- Patient lost to follow-up.
Criteria for Evaluation Safety Evaluations:
Safety will be assessed by vital sign measurements, clinical laboratory tests, ECG (for
patients ≥ 35 years of age) and routine physical examinations, including physical growth for
children up to 18 years old and the incidence and severity of adverse events (graded
according to CTCAE v 4.0).
Activity Evaluations:
Activity of TP10 in C3G will be assessed via complement studies (including but not limited
to serum C3, serum C3 breakdown products, and alternate pathway activity), chronic kidney
disease stage, renal biopsy (C3 deposition in the glomerular basement membrane), and renal
function (proteinuria, serum creatinine).
Pharmacokinetic Evaluations:
Serum concentrations of TP10 will be measured concurrently with serum C3, C3 breakdown
products, and alternative pathway complement activity in samples taken immediately before
and approximately 15 minutes after TP10 infusion. No pharmacokinetic parameters will be
determined in this study.
Immunological Evaluations:
Patients will be monitored for the development of antibodies to TP10.
Pharmacodynamic Evaluations:
Pharmacodynamics of TP10 will be assayed by changes in serum C3, serum C3 breakdown products
and alternative pathway complement activity.
Pharmacogenomic Evaluations:
Patients will undergo genetic testing of CFH, C3, CFB and CFHR5; assays for C3Nef activity;
and screening for factor H autoantibodies (FHAA) and factor B autoantibodies (FBAA).
single-arm, clinical trial of TP10 in 5 patients with C3G, aged 4 years or older. The study
consists of a 4-week screening period followed by a 26-week treatment period. (See Schedule
of Events, Table 1.) The 26-week treatment period is further divided into an Induction
Period of up to 4 weeks, followed by a Maintenance Period, which allows for continued
treatment to a total of 26 weeks.
Screening Period: Patients will be identified for possible enrollment in this study through
a number of mechanisms, including physician or patient-self referral and participation in an
on-going study of C3G in which renal pathology is reviewed to confirm the diagnosis of C3G
and genetic and complement studies are performed. Patients who appear to meet eligibility
criteria for this study upon initial review will be asked to contact Drs. Nester and Smith
if they are interested in this study. Those patients who express interest in this study will
be scheduled for a screening clinic visit at which time they will meet the study team and
review the study design and requirements. A consent for study participation will be
obtained. During this visit those events/tests noted on Table 1, Screening Visit, will be
completed. If not already vaccinated within the time period of active coverage specified by
the vaccine manufacturer, patients will be administered meningococcal, pneumococcal and
haemophilus influenzae vaccines prior to study drug administration.
Treatment Period: All patients will be enrolled through the University of Iowa. This study
will follow a patient-specific dose-escalation scheme during the Induction Period and
subsequent dose adjustments based on complement levels during the Maintenance Period (as
described under Investigational Product Dosing and Administration).
Safety Monitoring: Safety data for this trial will be reviewed by a Data Monitoring and
Safety Person (DMSP) consisting of one reviewer who is otherwise independent of trial
conduct, as well as study investigators. The DMSP will review safety data on a periodic
basis based on the accrual rate and emergence of safety data. The DMSP will evaluate patient
data with the purpose of identifying safety concerns that may require a modification of the
current study protocol and will also be responsible for determining if criteria for halting
of the trial are met (see below).
Study Stopping Rules: If any of the following criteria are met, further enrollment into the
trial will be halted and the data reviewed with the DMSP. The trial will only be reopened
after a mutually agreed plan is defined with the DMSP.
- Futility in the first three patients. Futility is defined as:
- Failure during the Induction Period to normalize C3, C3 breakdown products or
alternative pathway complement activity
- Any of the following toxicities in more than one patient:
- Dose-limiting toxicity (DLT), defined as any Grade 3 or higher drug-related
adverse event (AE)
- Grade 3 or higher infection caused by encapsulated bacteria, not responsive to
appropriate medical intervention within 24 hours
- Drug-related death Investigational Product Dosing and Administration Each TP10
administration will consist of a 60 (±5)-minute intravenous drip infusion using a 0.22
µm in-line filter and a controlled-rate infusion pump. Administered doses will range
from 5 mg/kg to 30 mg/kg, as determined by patient-specific dose-escalation and
adjustment. Any change in weight of more than 10% will require re-calculation of the
administered dose; otherwise, dosing may be based on the baseline weight. All dosing
will be bi-weekly during induction and weekly during maintenance.
To determine the effect of TP10 on complement and C3 convertase inhibition, complement
studies will include measuring TP10 serum concentrations and serum levels of C3 and C3
breakdown products and assays of alternative pathway function. Testing will be done on serum
and plasma samples obtained prior to and approximately 15 minutes post each TP10 dose. All
complement studies will be performed at the University of Iowa. The following treatment plan
will be followed for each patient. However, given the limited experience with TP10 in the
treatment of C3G, as well as the breadth of complement studies that may be used to assess
the impact of treatment, it is acknowledged that the treatment plan within this pilot study
may not account for all potential clinical scenarios. Therefore, adjustments to dose level
or frequency that fall outside of this plan may be implemented when determined clinically
appropriate by the lead investigators at the University of Iowa. In such cases, the IRB will
be notified of the plan for dose change.
Induction Period During the Induction Period, samples for complement studies will be
analyzed at least weekly. The first two doses of the Induction Period will be 5 mg/kg.
Intra-patient dose-escalation will subsequently occur weekly, in 5 or 10 mg/kg increments
(as determined by the investigator, based on complement biomarker changes), up to a maximum
dose of 30 mg/kg.
The Induction Period schedule will be modified when either of the following criteria are
met:
- Dose escalation will discontinue when normalization of C3, C3 breakdown products AND/OR
measure(s) of alternative and/or terminal pathway complement activity is achieved.
Thereafter, the patient will receive one additional TP10 dose at the same dose level as
the prior dose, and then transition to the Maintenance Period.
- If the dose level of 30 mg/kg is reached without normalization of C3, C3 breakdown
products AND/OR measure(s) of alternative and/or terminal pathway complement activity,
the patient may receive one additional dose of TP10 at 30 mg/kg.
- If normalization of C3, C3 breakdown products AND/OR measure(s) of alternative
and/or terminal pathway complement activity fails to occur, treatment will be
discontinued.
- If normalization of C3, C3 breakdown products AND/OR measure(s) of alternative
and/or terminal pathway complement activity occurs, the patient will enter the
Maintenance Period and follow rules for Maintenance Period dose adjustments.
In addition, study drug dosing will be discontinued if any additional criteria for
discontinuation of study therapy (see below) are met.
Maintenance Period
Since it is quite possible that the dose required for maintenance may be significantly lower
than that required during induction, the Maintenance Period will seek to identify the lowest
dose that provides ongoing control of undesirable complement activity. The starting dose for
TP10 Maintenance will be the same dose level as the last dose during the Induction Period;
however, the Maintenance Period allows for dose decrease to 2 mg/kg, which is lower than the
starting dose in the Induction Period. Samples for complement studies will be collected on
each dosing day and analyzed at least weekly at University of Iowa during the Maintenance
Period. Therefore, treatment decisions will be made at least weekly, and dose adjustments
throughout the Maintenance period will be implemented as follows (see Section 8.3.2 for
further details):
- If C3, C3 breakdown products AND/OR measure(s) of alternative and/or terminal pathway
complement activity are normalized for two consecutive weeks, the next Maintenance dose
may be decreased by 5 mg/kg (if the previous dose is 5 mg/kg, dosing will decrease to 2
mg/kg).
o Note: The dose level MAY be maintained if deemed appropriate by the treating
investigator, with consideration to factors such as biomarker evidence of neo-C3
convertase generation and overall profile of labs utilized for defining maintenance.
- If C3 levels have dropped >25% compared to entry into the Maintenance Period, C3
breakdown products are present (greater than normal), AND/OR measure(s) of alternative
or terminal pathway complement activity have significantly changed (>50% worsening in
value), the next Maintenance dose will be increased by 5 mg/kg up to a maximum of 30
mg/kg (if the previous dose is 2 mg/kg, dosing will increase to 5 mg/kg).
- If a patient has experienced dose reduction and subsequent dose escalation twice,
further dose reductions may not be required, but can be implemented at the
investigator's discretion. Otherwise, these patients may be maintained at the last dose
that provided normalization of C3, C3 breakdown products AND/OR alternative and/or
terminal pathway complement activity unless there are changes requiring a dose
increased, as described above.
- If normalization of C3, C3 breakdown products AND/OR alternative and/or terminal
pathway complement activity fails to occur despite receipt of 30 mg/kg twice weekly
dosing for two weeks, the patient will be withdrawn from the study.
The Maintenance Period will be continued until either:
- The total study treatment period of 26 weeks has elapsed;
- Any additional criteria for discontinuation of study therapy (see below) are met.
Additional criteria for treatment discontinuation
At any point during the study, treatment will be discontinued for any of the following
reasons:
- Decrease in renal function, defined by an increase in serum creatinine by 50% over
baseline (last assessment prior to first TP10 dose), persistent for 4 weeks.
- Development of dose-limiting toxicity (DLT), defined as any Grade 3 or higher AE
attributed to TP10 dosing, or any Grade 3 infection caused by encapsulated bacteria,
not responsive to appropriate medical intervention within 24 hours. Patients who
experience DLT but who are considered by the treating investigator to be potentially
appropriate for further TP10 treatment may be retreated only after consultation with,
and agreement from, the DMSP.
- The study is terminated (see early stopping rules).
- Request of the patient or the patient's legal representative.
- If, in the investigator's medical judgment, further participation would be injurious to
the patient's health or wellbeing.
- Non-compliance of the patient.
- Pregnancy.
- Patient lost to follow-up.
Criteria for Evaluation Safety Evaluations:
Safety will be assessed by vital sign measurements, clinical laboratory tests, ECG (for
patients ≥ 35 years of age) and routine physical examinations, including physical growth for
children up to 18 years old and the incidence and severity of adverse events (graded
according to CTCAE v 4.0).
Activity Evaluations:
Activity of TP10 in C3G will be assessed via complement studies (including but not limited
to serum C3, serum C3 breakdown products, and alternate pathway activity), chronic kidney
disease stage, renal biopsy (C3 deposition in the glomerular basement membrane), and renal
function (proteinuria, serum creatinine).
Pharmacokinetic Evaluations:
Serum concentrations of TP10 will be measured concurrently with serum C3, C3 breakdown
products, and alternative pathway complement activity in samples taken immediately before
and approximately 15 minutes after TP10 infusion. No pharmacokinetic parameters will be
determined in this study.
Immunological Evaluations:
Patients will be monitored for the development of antibodies to TP10.
Pharmacodynamic Evaluations:
Pharmacodynamics of TP10 will be assayed by changes in serum C3, serum C3 breakdown products
and alternative pathway complement activity.
Pharmacogenomic Evaluations:
Patients will undergo genetic testing of CFH, C3, CFB and CFHR5; assays for C3Nef activity;
and screening for factor H autoantibodies (FHAA) and factor B autoantibodies (FBAA).
Inclusion Criteria:
1. Patient must have C3G as confirmed by renal biopsy within six months of enrollment
(confirmation by University of Iowa investigators is required). If the patient is
post transplant, the repeat renal transplant biopsy must show C3 dominant
glomerulonephritis, and the patient must have a history of known C3G in the native
kidney.
2. C3 serum must be less than 75% of the lower limit of normal.
3. Signs of alternative pathway dysregulation must be present. C3 breakdown products or
C3Nef activity must be detectable in plasma using assays described and validated at
the University of Iowa
4. Serum creatinine level must be abnormal (>97 percentile for age or <80 ml/min using
the Cockroft Gault equation for adults).
5. Must have either 24 hour urine protein >1000 mg/day, or urine protein:creatinine
ratio >1.0.
6. Screening laboratory values must meet the following criteria:
- hemoglobin ≥ 9.0 g/dL
- platelet count ≥ 100,000/mm3
- alanine transaminase (ALT) and aspartate transaminase (AST) ≤ 3.0 x ULN
7. Must use adequate birth control measures.
8. Patient must be willing and able to comply with study procedures including
vaccination against meningitis, haemophilus and pneumococci at least 2 weeks prior to
starting the Induction Period and agree to a renal biopsy at the conclusion of the
study.
9. Any anti-proteinuric medications (eg, angiotensin converting enzyme inhibitors,
angiotensin II receptor blockers) must be at a stable dose for at least four weeks
prior to first dose of TP10.
Exclusion Criteria:
1. Dialysis or patients with an estimated glomerular filtration rate (eGFR; using
Cockroft Gault equation) of less than 30 ml/min/1.73 m2 for over a four-week period
prior to the Screening Period
2. Presence or suspicion of active or untreated systemic bacterial infection that in the
opinion of the investigator precludes treatment with TP10
3. Pregnancy or lactation
4. Rituximab therapy, unless discontinued with B cell levels and immunoglobulin levels
normalized by study entry
5. Patients receiving immunosuppressive therapies (except for low dose steroids [≤10 mg
of prednisone or equivalent per day] given for non-C3G related conditions such as
asthma). Patients receiving steroids for C3G must complete a taper prior to study
entry. Exceptions will be made for renal transplant patients, who may receive any
appropriate therapies as needed to maintain the transplant (i.e., to prevent
rejection).
6. Receipt of any complement inhibitor within 2 months of study entry
7. Receipt of any other investigational drug or device or experimental procedures
beginning four weeks prior to study enrollment
8. For renal transplant patients only: histology findings of treatable rejection (i.e.
that the usual transplant physician would seek to treat). Chronic allograft
nephropathy is not exclusionary provided the patient's GFR meets other entry
criteria.
9. A preexisting condition with a reported association as a potential cause of C3G
(i.e., Monoclonal Gammopathy of Undetermined Significance [MGUS]) or an alternate
glomerular disease that may interfere with the interpretation of study results
10. Malignancy except for adequately treated and cured basal or squamous cell skin
cancer, curatively treated in situ disease, or other cancer from which the patient
has been disease-free for ≥ 5 years
11. Patients with myocardial infarction (MI) within 1 year of screening, congestive heart
failure, arrhythmia persistent on medication at screening or clinically evident
chronic lung disease
12. Known Human Immunodeficiency Virus (HIV), Hepatitis B or Hepatitis C infection
13. Any medical or psychological condition that, in the opinion of the investigator,
would increase the patient's risk by participation in this study or would interfere
with interpretation of the study
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