Autoantibody Reduction for Acute Exacerbations of Idiopathic Pulmonary Fibrosis



Status:Recruiting
Conditions:Pulmonary
Therapuetic Areas:Pulmonary / Respiratory Diseases
Healthy:No
Age Range:40 - 85
Updated:9/7/2018
Start Date:September 4, 2018
End Date:September 30, 2022
Contact:Steven R Duncan, MD
Email:srduncan@uabmc.edu
Phone:205-934-5018

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Study of Therapeutic Plasma Exchange, Rituximab and Intravenous Immunoglobulin for Acute Exacerbations of Idiopathic Pulmonary Fibrosis (STRIVE-IPF)

Acute exacerbations (AE) are a dreaded manifestation of idiopathic pulmonary fibrosis (IPF)
that presents with rapidly worsening respiratory function over days to weeks. AE account for
about 1/2 the deaths in IPF patients, and are refractory to all medical therapies attempted
to date.

Considerable preliminary data shows pathological B-cell abnormalities and autoantibodies are
present in AE-IPF and associated with disease severity.

The experimental therapy here (therapeutic plasma exchange plus rituximab plus intravenous
immunoglobulin) is mechanistically targeted to ameliorate autoantibody-mediated pulmonary
injury. Anecdotal pilot studies indicate these treatments have significant benefit for a
disease syndrome that has, until now, been almost invariably inexorable. This clinical trial
has the potential to profoundly affect current paradigms and treatment approaches to patients
with AE-IPF.

The primary goal of clinical trial is to determine effects of combined therapeutic plasma
exchange (TPE), rituximab, and intravenous immunoglobulin (IVIG) in comparison to effects of
treatment as usual (TAU), among AE-IPF patients.

Our central hypothesis is "AUTOANTIBODY REDUCTION IS BENEFICIAL FOR AE-IPF PATIENTS." A
corollary of this hypothesis is that antibody-mediated autoimmunity can play an important
role in IPF exacerbations.

Following baseline screening assessments, hospitalized AE-IPF patients at the collaborating
sites that meet all inclusion/exclusion criteria will be randomly assigned to receive one of
the following treatments in a ratio of 2:1:

• Arm A (n=34) - Experimental Treatment:

Steroids: Prednisone 60 mg (p.o.) on day 1, followed by 20 mg/day on days 2-5, 7-14, and
16-19 (or the i.v. methylprednisolone equivalent). Methyl-prednisolone 100 mg i.v. will be
administered on days 6 and 15, as a premedication prior to the rituximab.

Insertion of a dialysis/apheresis catheter into a central vein, and initiation of therapeutic
plasma exchange (TPE), rituximab, and intravenous immunoglobulin (IVIG) regimens:

Therapeutic Plasma Exchange (TPE) will consist of 1x estimated plasma volume exchanges for 3
successive days (1-3) and then, after a one day interval to enable equilibration of
autoantibodies between intra- and extra-vascular spaces, again on days 5, 6, 9, 11, 13, and
15.

Rituximab: One gm i.v. will be administered on day 6 and day 15 after completion of the TPE
on those days.

Intravenous immunoglobulin (IVIG): 0.5 gm/kg/day i.v. on days 16-19

• Arm B (n=17) - Treatment as Usual (TAU):

The same steroid regimen as described for Arm A, i.e., prednisone 60 mg (p.o.) on day 1,
followed by 20 mg/day on days 2-5, 7-14, and 16-19 (or the i.v. methylprednisolone
equivalent), and methylprednisolone 100 mg i.v. administered on days 6 and 15.

All patients enrolled in both cohorts at all sites will also receive empiric broad-spectrum
antibiotics for 8 days. The empiric antibiotic regimen will be reassessed and tailored based
on any subsequent cultures and sensitivity results.

Patients will be monitored carefully for occurrences of adverse events, laboratory test
abnormalities, and changes in vital signs.

The respective treatment courses can be finished on an outpatient basis among enrolled
patients who are able to be discharged from the hospital, if medically indicated, and if
those treatment compliance can be assured.

Patients will be followed for the duration of their hospital admission after enrollment, and
then observed as either inpatients or outpatients on days 19, 60, 90, 180, 270, and 365. A
telephone contact will occur at monthly intervals, aside from those visits above. The total
observation/subject is 365 days.

Inclusion Criteria:

1. Age between 40-85 years old.

2. A diagnosis of IPF that fulfills ATS/ERS Consensus Criteria.1

3. Worsening or new development of dyspnea or hypoxemia within the last 30 days.

4. Ground-glass abnormality and/or consolidation superimposed on a reticular or honeycomb
usual interstitial pneumonitis (UIP) pattern on locally read chest CT scan.

5. Ability and willingness to give informed consent (no surrogates) and adhere to study
requirements.

Exclusion Criteria:

1. Diagnoses of current infection per clinical or microbial assessments.

2. Diagnoses of an additional or alternative etiology for respiratory dysfunction based
upon clinical assessment, including congestive heart failure, sepsis, thromboembolism,
etc.

3. History or serologic evidence of hepatitis B or C infection.

4. Coagulopathy, defined as a International Normalized Ratio (INR) >1.6, partial
thromboplastin time (PTT) > 2x control, fibrinogen <100 mg/dL, or platelet count <50
thousand (K) unless these abnormalities can be reversed safely.

5. Hyperosmolar state or diabetic ketoacidosis to suggest uncontrolled diabetes, or
uncontrolled hypertension (systolic BP >160 mm Hg and diastolic BP >100 mm Hg) that
would contraindicate use of corticosteroids.

6. Hemodynamic instability, defined as an inotrope or vasopressor requirement.

7. History of reaction to blood products or murine-derived products or prior rituximab
use.

8. History of malignancy, excluding basal or squamous cell skin cancer and low-risk
prostate cancer, the latter defined as stage T1 or T2a, with prostate specific antigen
(PSA) less than 10 ng/dl. The experimental treatments are not known to promote cancer
progression, and these criteria are within current guidelines.

9. Unwillingness to accept blood product transfusion.

10. Diagnosis of major comorbidities expected to interfere with study participation.

11. Treatment for >14 days within the preceding month with >20 mg. prednisone (or
equivalent) or any treatment during the last month with a cellular immuno-suppressant
(e.g., cyclophosphamide, methotrexate, calcineurin inhibitors, mycophenolate,
azathioprine, etc.). An exception will be made if the patient has a bronchoalveolar
lavage (BAL) negative for pathogens.

12. Current treatment with an angiotensin converting enzyme inhibitor that cannot be
discontinued and/or substituted (to obviate hemodynamic complications during TPE).

13. Concurrent participation in other experimental trials.

14. Fertile females who do not agree to contraception or abstinence, or have a positive
pregnancy test (urine or blood). IPF is a disease of older adults, and male
predominant, so this will not be a frequent consideration.

15. Presence of positive (abnormal) classical autoimmune tests: anti-nuclear antibody
(ANA), rheumatoid factor (RF), Anti- Sjögren's-syndrome-related antigen (SSA) , and
Anti-Cyclic Citrullinated Peptide (CCP). This criterion will eliminate patients with
confounding classical autoimmune syndromes. Many IPF patients will have already had
these tests, which are standard of practice (SOP) at many IPF centers, and these prior
results will suffice if the tests were performed within the last year. Otherwise,
these tests need to be performed prior to enrollment and they can usually be procured
in 1-2 days. Based on experience, we anticipate ~10% of patients who fulfill all other
IPF criteria will nonetheless be positive for one of these classical autoantibody
tests.

16. IgA deficiency (IgA level <7 mg/dL)- to preclude IVIG reactions.
We found this trial at
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200 Lothrop St
Pittsburgh, Pennsylvania 15213
Phone: 412-802-3275
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1720 2nd Ave S
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75 Francis street
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3401 N Broad St
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