The Effect of Vitamin C on Wound Healing In Mandibular Fracture Patients
Primary Purpose
Vitamin C Deficiency, Smoking, Surgery
Status
Completed
Phase
Not Applicable
Locations
United States
Study Type
Interventional
Intervention
Vitamin C
Placebo
Sponsored by
About this trial
This is an interventional treatment trial for Vitamin C Deficiency
Eligibility Criteria
Inclusion Criteria:
- patients age 18 or older with de novo mandibular fracture undergoing surgical repair with an intra-oral incision based approach with plating (ie- not solely mandibular maxillary fixation which requires no surgical incision).,
- surgery within 7 days of injury.
Exclusion Criteria:
- cognitive impairment limiting ability to provide informed consent
- pregnancy or nursing
- a known history of renal insufficiency
- comminuted fractures,
- allergy to Vitamin C / placebo components.
- Isolated subcondylar fractures
Sites / Locations
- Hennepin Healthcare Research Institute
Arms of the Study
Arm 1
Arm 2
Arm Type
Experimental
Placebo Comparator
Arm Label
Vitamin C
Placebo
Arm Description
Outcomes
Primary Outcome Measures
Procollagen I
Biomarker of soft tissue repair. Measured in picogram/milliliter (pg/ml) in blood serum.
Procollagen III
Biomarker of soft tissue repair. Measured in picogram/milliliter (pg/ml) in blood serum.
Secondary Outcome Measures
Matrix Metallo-Proteinases 1,2,3 & 9
Biomarker of soft tissue repair. Measured in picogram/milliliter (pg/ml) in blood
C-reactive protein
Biomarker of soft tissue repair. Measured in nanogram/milliliter (ng/ml) in blood
Neutrophil count
Biomarker of soft tissue repair. Measured in picogram/milliliter (pg/ml) in blood
Interleukins 6 & 8
Biomarker of soft tissue repair. Measured in picogram/milliliter (pg/ml) in blood
Thiobarbituric acid reactive substances
Biomarker of soft tissue repair. Measured in micro Molar uM in blood
Trolox equivalent antioxidant capacity
Biomarker of soft tissue repair. Measured in nanomol/microliter (nmol/ul) in blood
alkaline phosphatase
Biomarker of bone repair. Measured in enzyme unit/liter (U/L) in blood
Tartrate Resistant Acid Phosphatase 5b
Biomarker of bone repair. Measured in enzyme unit/liter (U/L) in blood
osteocalcin
Biomarker of bone repair. Measured in picogram/milliliter (pg/ml) in blood
osteoprotegerin
Biomarker of bone repair. Measured in picogram/milliliter (pg/ml) in blood
carboxy terminal collagen crosslinks
Biomarker of bone repair. Measured in nanogram/milliliter (ng/ml) in blood
Receptor activator of nuclear factor kappa-B ligand
Biomarker of bone repair. Measured in picogram/milliliter (pg/ml) in blood
Vitamin C
Vitamin C levels. Measured in nanomols (nmmol) in blood serum
Cotinine
Biomarker of tobacco exposure. Measured in nanograms/milliliter (mg/ml) in blood serum.
Full Information
NCT ID
NCT03938584
First Posted
April 26, 2019
Last Updated
January 25, 2022
Sponsor
Hennepin Healthcare Research Institute
Collaborators
Regions Hospital, University of Minnesota
1. Study Identification
Unique Protocol Identification Number
NCT03938584
Brief Title
The Effect of Vitamin C on Wound Healing In Mandibular Fracture Patients
Official Title
The Effect of Vitamin C on Wound Healing In Mandibular Fracture Patients: A Double Blind, Placebo-controlled Randomized Clinical Trial
Study Type
Interventional
2. Study Status
Record Verification Date
January 2022
Overall Recruitment Status
Completed
Study Start Date
October 12, 2017 (Actual)
Primary Completion Date
June 1, 2021 (Actual)
Study Completion Date
June 1, 2021 (Actual)
3. Sponsor/Collaborators
Responsible Party, by Official Title
Sponsor
Name of the Sponsor
Hennepin Healthcare Research Institute
Collaborators
Regions Hospital, University of Minnesota
4. Oversight
Studies a U.S. FDA-regulated Drug Product
No
Studies a U.S. FDA-regulated Device Product
No
Data Monitoring Committee
No
5. Study Description
Brief Summary
The goal of this study is to perform a randomized clinical trial to assess the effects of vitamin C versus placebo on wound healing in mandibular fracture patients.
Detailed Description
In a prospective, randomized clinical trial of de novo mandibular fracture patients requiring intraoral surgical repair with plating, the investigators will:
Compare the effects of supplemental vitamin C to placebo on soft tissue wound healing, measured by a) biomarkers of soft tissue repair (Procollagen I and III, Matrix Metallo-Proteinases 1,2,3 & 9, C-reactive protein, neutrophil count, Interleukins 6 & 8, TBARS and TEAC) and b) clinical outcomes (wound dehiscence and Wound Score).
Hypothesis1: Supplemental vitamin C will improve soft tissue healing post-mandibular fracture, measured by improved procollagen I, other biomarker levels and clinical outcomes, compared to placebo.
Rationale. The clinical literature describes impaired soft tissue wound healing in mandibular fracture patients, including wound infection, wound dehiscence, and plate exposure. Vitamin C is a necessary co-factor for the production of types I and III collagen, as well as procollagen, the precursor to collagen, via the hydroxylation of proline and lysine. In the setting of vitamin C deficiency, collagen production is abnormal leading to defective vessel and connective tissue formation with degradation of unstable collagen molecules.90-91,34, 63, 108,109
The investigators will collect a robust set of clinical outcomes including clinician evaluation and Wound Healing Score to measure soft tissue healing. Biomarkers of soft tissue wound healing will be used to measure biochemical healing pathways as well. As a precursor to collagen, procollagen I and III are widely used biomarkers of collagen production in wound healing research. The investigators will assess these levels at baseline and at 3 to 5weeks post-operatively to evaluate the effect of vitamin C on collagen production. In addition, the antioxidant effects of vitamin C are critical during the ordered phases of wound healing, from the inflammatory phase (including the initial hemostatic cascade) to the proliferative phase. Antioxidant depletion during these phases results in imbalanced proteolytic enzyme cascades (including matrix metalloproteinases or MMPs) with resulting tissue destruction as well as an over-exuberant inflammatory milieu. Further, the antioxidant deficit resulting from vitamin C deficiency results in diminished monocyte and neutrophil chemotaxis and diminished bacteriocidal oxidative burst capabilities. Thus, the investigators will additionally measure the effects of vitamin C supplementation on proteolytic enzyme pathways (MMPs) and systemic markers of infection and inflammation (neutrophil count, c-reactive protein level, interleukins (IL) 1 and 6). Finally, the investigators will use indicators of oxidative stress at baseline and 6 weeks to measure the effects of vitamin C supplementation on antioxidant capacity (TBARS and TEAC).
Compare the effects of supplemental vitamin C to placebo on bone repair, measured by a) biomarkers of bone repair (alkaline phosphatase, TRACP 5b, osteocalcin, RANKL, osteoprotegerin, and carboxy terminal collagen crosslinks) and b) clinical outcomes (radiologic imaging and pain).
Hypothesis 2: Supplemental vitamin C will improve bone healing post-mandibular fracture, measured by improved biomarkers of bone healing and more robust radiological bone imaging, compared to placebo.
Rationale. A body of literature, from animal studies to randomized clinical trials, supports the notion that vitamin C is necessary for bone health and healing. Multiple animal studies demonstrate that vitamin C promotes bone formation / mineralization, strengthens developing callous, and supports bone maintenance. Further, a number of studies show that supplemental vitamin C prevents fracture in menopausal women and may be protective against arthritis.10,11,12,69 Several well done randomized controlled clinical trials have shown that supplemental vitamin C diminishes regional pain syndrome after distal radius fractures and less robust data suggests this for foot and ankle fractures. Well-done randomized controlled clinical trials are needed to develop Vitamin C guidelines in traumatic facial fracture.
The investigators will collect a comprehensive set of biochemical, clinical, and radiological outcome measures to evaluate bony healing after mandibular fracture. The biomarker evaluation will include assessment of osteoblast and osteoclast number (alkaline phosphatase and TRACP 5b respectively), osteoblast activity (osteocalcin), osteoclast differentiation (receptor activator for nuclear factor, B ligand or RANKL and osteoprotegerin or decoy receptor for RANKL) and osteoclast activity (carboxy terminal collagen crosslinks). The investigators will measure clinical outcomes about 1 and 3 to 5 weeks postoperatively. Finally, each subject will undergo a non-contrast CT of the mandible 3to 5 weeks post-operatively for radiological evaluation of bone healing. The CT scan may or may not be standard of care.30,36,135
Determine the effects of supplemental vitamin C on soft tissue and bone healing by smoking status in patients with traumatic mandibular fracture.
Hypothesis 3: Current smokers will have a higher prevalence of vitamin C deficiency than nonsmokers at baseline, and vitamin C supplementation will improve soft tissue and bone healing more in smokers than nonsmokers.
Rationale. Despite clinical evidence for smoking-related impairment in wound healing, much is unknown about the pathophysiologic mechanisms underlying this effect.21. It is postulated that after injury, smoking impedes the inflammatory phase of wound healing by diminishing cellular chemotactic responsiveness, migratory function, and oxidative bacterial killing, and by creating an imbalance in protease-protease inhibitor relationships. The proliferative phase of wound healing is also potentially impaired by smoking, with diminished fibroblast proliferation and migration resulting in decreased collagen production.124-30 Increases in oxidative stress and hypoxia further diminish healing in smokers.62,74,76,102 Vitamin C is postulated to be an important contributor to the diminished wound healing evidenced in smokers. Both population and experimental studies have shown smokers are more likely to be deficient in Vitamin C, with 25% of female smokers and 30% of male smokers having severe deficiency. This deficiency is likely secondary to a systemic depletion by the many reactive oxygen species in tobacco smoke as well as a diet lacking antioxidants. The investigators will evaluate the effects of vitamin C on wound healing in current versus non smokers with detailed assessment of tobacco use.
This project assembles a multidisciplinary team with expertise in wound healing, maxillofacial surgery, medical effects of tobacco use, fracture repair, biomechanics of bone, and conduct of clinical trials. The proposed work will define specific effects of supplemental Vitamin C on soft tissue and bone healing, with additional attention to smoking status in patients with mandibular fractures. For the many patients who are at high risk for vitamin C deficiency and poor wound healing, this investigation will provide critical knowledge of the role of oxidative stress and anti-oxidants in the mechanisms of impaired healing. These data will provide pilot data to support randomized controlled trials of interventions to improve post-operative wound healing in patients suffering from mandibular and other traumatic fractures. Establishing the safety and efficacy of supplemental Vitamin C in the peri-operative setting will improve wound healing outcomes for thousands of patients undergoing traumatic fracture surgery and could be a transformative step in treatment guidelines for any smoker undergoing surgery.
6. Conditions and Keywords
Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Vitamin C Deficiency, Smoking, Surgery, Surgery--Complications, Wound, Wound Complication, Wound Infection, Wound Dehiscence, Wound of Skin, Mandible Fracture, Mandible Open Fracture, Mandible Closed Fracture, Mandibular Fractures, Ascorbic Acid Deficiency, Oxidative Stress, Inflammation
7. Study Design
Primary Purpose
Treatment
Study Phase
Not Applicable
Interventional Study Model
Parallel Assignment
Masking
ParticipantCare ProviderInvestigatorOutcomes Assessor
Allocation
Randomized
Enrollment
45 (Actual)
8. Arms, Groups, and Interventions
Arm Title
Vitamin C
Arm Type
Experimental
Arm Title
Placebo
Arm Type
Placebo Comparator
Intervention Type
Dietary Supplement
Intervention Name(s)
Vitamin C
Other Intervention Name(s)
Ascorbic Acid
Intervention Description
Just after induction of anesthesia in the OR, subjects will be administered a single intravenous (IV) dose of Vitamin C at 66mg/kg/hr for 2 hours during surgery. Post-operatively (beginning the morning after surgery) Vitamin C Treatment Group subjects will receive a 4 week prescription of oral, liquid Vitamin C, 500mg by mouth two times a day. These dosages are known to be safe and effective.89-91
Intervention Type
Other
Intervention Name(s)
Placebo
Intervention Description
Subjects will receive IV placebo (normal saline) identically packaged. Post-operatively Placebo Control Treatment Group participants will receive a 4-week prescription of the aqueous solution base used for the treatment group without the active component (Vitamin C).
Primary Outcome Measure Information:
Title
Procollagen I
Description
Biomarker of soft tissue repair. Measured in picogram/milliliter (pg/ml) in blood serum.
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Title
Procollagen III
Description
Biomarker of soft tissue repair. Measured in picogram/milliliter (pg/ml) in blood serum.
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Secondary Outcome Measure Information:
Title
Matrix Metallo-Proteinases 1,2,3 & 9
Description
Biomarker of soft tissue repair. Measured in picogram/milliliter (pg/ml) in blood
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Title
C-reactive protein
Description
Biomarker of soft tissue repair. Measured in nanogram/milliliter (ng/ml) in blood
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Title
Neutrophil count
Description
Biomarker of soft tissue repair. Measured in picogram/milliliter (pg/ml) in blood
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Title
Interleukins 6 & 8
Description
Biomarker of soft tissue repair. Measured in picogram/milliliter (pg/ml) in blood
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Title
Thiobarbituric acid reactive substances
Description
Biomarker of soft tissue repair. Measured in micro Molar uM in blood
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Title
Trolox equivalent antioxidant capacity
Description
Biomarker of soft tissue repair. Measured in nanomol/microliter (nmol/ul) in blood
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Title
alkaline phosphatase
Description
Biomarker of bone repair. Measured in enzyme unit/liter (U/L) in blood
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Title
Tartrate Resistant Acid Phosphatase 5b
Description
Biomarker of bone repair. Measured in enzyme unit/liter (U/L) in blood
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Title
osteocalcin
Description
Biomarker of bone repair. Measured in picogram/milliliter (pg/ml) in blood
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Title
osteoprotegerin
Description
Biomarker of bone repair. Measured in picogram/milliliter (pg/ml) in blood
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Title
carboxy terminal collagen crosslinks
Description
Biomarker of bone repair. Measured in nanogram/milliliter (ng/ml) in blood
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Title
Receptor activator of nuclear factor kappa-B ligand
Description
Biomarker of bone repair. Measured in picogram/milliliter (pg/ml) in blood
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Title
Vitamin C
Description
Vitamin C levels. Measured in nanomols (nmmol) in blood serum
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Title
Cotinine
Description
Biomarker of tobacco exposure. Measured in nanograms/milliliter (mg/ml) in blood serum.
Time Frame
Blood is obtained the day of surgery and 6 weeks after surgery
Other Pre-specified Outcome Measures:
Title
Wound score
Description
Wounds are scored from photographs using the InCISE wound score developed by the investigator.
Time Frame
Wounds are analyzed 1 week and 6 weeks after surgery.
10. Eligibility
Sex
All
Minimum Age & Unit of Time
18 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria:
patients age 18 or older with de novo mandibular fracture undergoing surgical repair with an intra-oral incision based approach with plating (ie- not solely mandibular maxillary fixation which requires no surgical incision).,
surgery within 7 days of injury.
Exclusion Criteria:
cognitive impairment limiting ability to provide informed consent
pregnancy or nursing
a known history of renal insufficiency
comminuted fractures,
allergy to Vitamin C / placebo components.
Isolated subcondylar fractures
Facility Information:
Facility Name
Hennepin Healthcare Research Institute
City
Minneapolis
State/Province
Minnesota
ZIP/Postal Code
55415
Country
United States
12. IPD Sharing Statement
Plan to Share IPD
No
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The Effect of Vitamin C on Wound Healing In Mandibular Fracture Patients
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