Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT03426761 |
| Other study ID # |
IIT-2017-10117 |
| Secondary ID |
|
| Status |
Completed |
| Phase |
Phase 4
|
| First received |
|
| Last updated |
|
| Start date |
January 25, 2018 |
| Est. completion date |
December 31, 2022 |
Study information
| Verified date |
October 2023 |
| Source |
Infectious Diseases Physicians, Inc. |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Because of its prolonged terminal half-life, dalbavancin is an extremely attractive option in
treating Gram-positive infections caused by S. aureus including MRSA, and streptococcal
species. Systemic bacterial infections due to Staphylococci such as osteomyelitis and septic
arthritis, are conditions which require prolonged IV therapy, typically for at least 3-6
weeks, though sometimes more. Due to dalbavancin's prolonged terminal half-life, it may offer
the opportunity to substantially reduce costs and morbidity in native joint and prosthetic
joint infections with one infusion every fourteen days until completion of therapy.
Description:
Dalbavancin, currently FDA approved for the treatment of skin and soft tissue infections
(SSTI), is a lipoglycopedptide with bactericidal activity in vitro against Staphylococcus
aureus, including MRSA and VISA strains, and Streptococcus pyogenes. Its bactericidal action
results primarily from inhibition of cell-wall biosynthesis, specifically the prevention of
N-acetylmuramic acid (NAM) and N-acetylglucosamine (NAG)-peptide subunits incorporation into
the peptidoglycan matrix. Dalbavancin alters bacterial-cell-membrane permeability and RNA
synthesis. It is highly protein bound, primarily to albumin, with a half-life of 346 hours.
Approximately 33% of unchanged drug is excreted in the urine, 20% via feces and 12% as the
minor metabolite, hydroxyl-dalbavancin. There is minimal potential for drug-drug
interactions; it is not a substrate, inducer or inhibitor of hepatic CYP450 isoenzymes and
the administration of CYP450 substrates, inhibitors or inducers does not affect its clearance
rate. In SSTI trials, Dalbavancin was demonstrated to be non-inferior to vancomycin and
linezolid.
Prosthetic joint infections (PJI) are an emerging health problem. Although the incidence of
these infections is historically low (approximately 0.5%-1.0of implants), because of the
rapid increase in the number of hip, knee and other joint implants, the absolute number of
cases of infection is increasing. In 2010, 332,000 hip joints and 719,000 knee joints were
implanted. This alone conservatively translates to 5,000-10,000 cases, with an economic
impact of $1 billion. Management of PJI is particularly challenging because long term
antibiotic therapy in most cases is accompanied by removal of the prosthesis and
re-implantation.
For long term antimicrobial administration, current standard of care requires a peripherally
inserted central catheter (PICC) or other indwelling intravascular catheter, and
daily/multiple daily infusions. There is substantial cost of maintaining the intravascular
access, drugs, home health care and monitoring, as well as the infection risk of the chronic
indwelling line which is being accessed frequently. There is a clear need for alternative
care models to the current approach. Dalbavancin, because of its activity profile against
Gram-positive organisms and its pharmacokinetics which would allow weekly or every other week
dosing, is a favorable option. This option would eliminate the need for long term IV access,
because at most, weekly IV infusions would be performed.
In terms of bone infection, dalbavancin has favorable pharmacokinetic properties. A PK study
performed in subjects undergoing elective orthopedic surgery found that dalbavancin (dosed at
1000mg IV at enrollment and then 500mg weekly for up to 7 weeks) maintained levels in
cortical bone at bactericidal levels , at >50X the MIC of typical staphylococcal organism
(including MRSA). Animal studies in a rat osteomyelitis model also found that dalvabancin was
comparable to vancomycin. Because of these same PK properties, dalbavancin offers the
opportunity to substantially reduce costs and morbidity in native joint and prosthetic joint
infections.
This is a two-center, randomized, open label trial of dalbavancin versus standard intravenous
therapy control comparator in the treatment of subjects with gram positive native joint or
prosthetic joint infections. The primary outcome variable is clinical cure at day 42 after
start of treatment in all randomized patients. Safety and tolerability will also be assessed
throughout the study period via laboratory measurements and AE monitoring. Additionally,
clinical response will be measured by patient reported outcomes with change from baseline
symptoms and by Quality of Life questionnaire.
Eligible subjects with confirmed gram positive joint infections, will be randomized in a
ratio of 2:1 to receive open label dalbavancin or standard IV therapy. Standard IV therapy
will depend on the antibiotic susceptibility of the causative pathogen. Subjects randomized
to dalbavancin may have received standard of care therapy for no more than 120 hours prior to
first dalbavancin dose. Subjects randomized to standard of care can continue with treatment
course if already started, or receive the first dose at the baseline visit.
