59 results on '"Moffatt, Lauren T."'
Search Results
2. American Burn Association (ABA) Burn Care Quality Platform (BCQP) and Large Data Set Analysis Considerations: A Practical Guide to Investigating Clinical Questions in Burns via Large Data Sets.
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Galicia, Kevin E, Thompson, Callie M, Lewis, Aislinn E, Joyce, Cara J, Hill, David M, Schneider, Jeffery C, Nyygard, Rachel M, Harrington, David M, Holmes, James H, Moffatt, Lauren T, Shupp, Jeff W, and Kubasiak, John C
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BIG data ,BURN care units ,BANKING industry ,TRAUMA registries ,DATA analysis - Abstract
The Burn Care Quality Platform (BCQP) consolidates data previously collected from the National Burn Repository and the Burn Quality Improvement Program into a single registry. Its data elements and their associated definitions are tailored to create consistency across other national trauma registries, namely the National Trauma Data Bank implemented by the American College of Surgeons Trauma Quality Improvement Program (ACS TQIP). The BCQP now includes 103 participating burn centers and has captured data from 375,000 total patients as of 2021. With 12,000 patients entered under the current data dictionary, the BCQP represents the largest registry of its kind. On behalf of the American Burn Association Research Committee, the aim of this whitepaper is to provide a succinct overview of the BCQP, showcasing its unique features, strengths, limitations, and relevant statistical considerations. This whitepaper will highlight the resources available to the burn research community and offer insight on proper study design when preparing to conduct a large data set investigation for burn care. All recommendations herein were formulated through the consensus of a multidisciplinary committee and based on the available scientific evidence. [ABSTRACT FROM AUTHOR]
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- 2024
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3. Treatment of hypopigmented burn hypertrophic scars with short‐term topical tacrolimus does not lead to repigmentation.
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Molina, Esteban A., Travis, Taryn E., Hussein, Lou'ay, Oliver, Mary A., Keyloun, John W., Moffatt, Lauren T., Shupp, Jeffrey W., and Carney, Bonnie C.
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- 2024
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4. Comparison of Rapid-, Kaolin-, and Native-TEG Parameters in Burn Patient Cohorts With Acute Burn-induced Coagulopathy and Abnormal Fibrinolytic Function.
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Keyloun, John W, Le, Tuan D, Moffatt, Lauren T, Orfeo, Thomas, McLawhorn, Melissa M, Bravo, Maria-Cristina, Tejiram, Shawn, Group, the SYSCOT Study, Shupp, Jeffrey W, and Pusateri, Anthony E
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BURN patients ,BLOOD coagulation disorders ,FIBRINOLYSIS ,BLOOD sampling ,THROMBELASTOGRAPHY - Abstract
Although use of thromboelastography (TEG) to diagnose coagulopathy and guide clinical decision-making is increasing, relative performance of different TEG methods has not been well-defined. Rapid-TEG (rTEG), kaolin-TEG (kTEG), and native-TEG (nTEG) were performed on blood samples from burn patients presenting to a regional center from admission to 21 days. Patients were categorized by burn severity, mortality, and fibrinolytic phenotypes (Shutdown [SD], Physiologic [PHYS], and Hyperfibrinolytic [HF]). Manufacturer ranges and published TEG cutoffs were examined. Concordance correlations (Rc) of TEG parameters (R, α-angle, maximum amplitude [MA], LY30) measured agreement and Cohen's Kappa (κ) determined interclass reliability. Patients (n = 121) were mostly male (n = 84; 69.4%), with median age 40 years, median TBSA burn 13%, and mortality 17% (n = 21). Severe burns (≥40% TBSA) were associated with lower admission α-angle for rTEG (P =.03) and lower MA for rTEG (P =.02) and kTEG (P =.01). MA was lower in patients who died (nTEG, P =.04; kTEG, P =.02; rTEG, P =.003). Admission HF was associated with increased mortality (OR, 10.45; 95% CI, 2.54–43.31, P =.001) on rTEG only. Delayed SD was associated with mortality using rTEG and nTEG (OR 9.46; 95% CI, 1.96–45.73; P =.005 and OR, 6.91; 95% CI, 1.35–35.48; P =.02). Admission TEGs showed poor agreement on R-time (Rc, 0.00–0.56) and α-angle (0.40 to 0.55), and moderate agreement on MA (0.67–0.81) and LY30 (0.72–0.93). Interclass reliability was lowest for R-time (κ, −0.07 to 0.01) and α-angle (−0.06 to 0.17) and highest for MA (0.22-0.51) and LY30 (0.29-0.49). Choice of TEG method may impact clinical decision-making. rTEG appeared most sensitive in parameter-specific associations with injury severity, abnormal fibrinolysis, and mortality. [ABSTRACT FROM AUTHOR]
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- 2024
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5. Neutrophil Extracellular Traps Are Induced by Coronavirus 2019 Disease-Positive Patient Plasma and Persist Longitudinally: A Possible Link to Endothelial Dysfunction as Measured by Syndecan-1.
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Kelly, Edward J., Oliver, Mary A., Carney, Bonnie C., Kolachana, Sindhura, Moffatt, Lauren T., and Shupp, Jeffrey W.
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- 2023
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6. Laser‐assisted drug delivery of synthetic alpha melanocyte stimulating hormone and L‐tyrosine leads to increased pigmentation area and expression of melanogenesis genes in a porcine hypertrophic scar model.
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Carney, Bonnie C., Oliver, Mary A., Kurup, Sanjana, Collins, Monica, Keyloun, John W., Moffatt, Lauren T., Shupp, Jeffrey W., and Travis, Taryn E.
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- 2023
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7. Endothelial damage occurs early after inhalation injury as measured by increased syndecan-1 levels.
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Kelly, Edward J, Carney, Bonnie C, Oliver, Mary A, Keyloun, John W, Prindeze, Nicholas J, Nisar, Saira, Moffatt, Lauren T, and Shupp, Jeffrey W
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INHALATION injuries ,SMOKE inhalation injuries ,SYNDECANS ,LUNG injuries ,BURN patients - Abstract
Inhalation injury is a significant cause of morbidity and mortality in the burn patient population. However, the pathogenesis of inhalation injury and its potential involvement in burn shock is not well understood. Preclinical studies have shown endothelial injury, as measured by syndecan-1 (SDC-1) levels, to be involved in the increased vascular permeability seen in shock states. Furthermore, the lung has been identified as a site of significant SDC-1 shedding. Here we aim to characterize the contribution of endotheliopathy caused by inhalation alone in a swine model. When comparing injured animals, the fold change of circulating SDC-1 levels from preinjury was significantly higher at 2, 4, and 6 hours postinjury (P =.0045, P =.0017, and P <.001, respectively). When comparing control animals, the fold change of SDC-1 from preinjury was not significant at any timepoint. When comparing injured animals versus controls, the fold change of SDC-1 injured animals was significantly greater at 2, 4, 6, and 18 hours (P =.004, P =.03, P <.001, and P =.03, respectively). Histological sections showed higher lung injury severity compared to control uninjured lungs (0.56 vs 0.38, P <.001). This novel animal model shows significant increases in SDC-1 levels that provide evidence for the connection between smoke inhalation injury and endothelial injury. Further understanding of the mechanisms underlying inhalation injury and its contribution to shock physiology may aid in development of early, more targeted therapies. [ABSTRACT FROM AUTHOR]
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- 2023
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8. Laser Treatment of Hypertrophic Scar in a Porcine Model Induces Change to Epidermal Histoarchitecture That Correlates to Improved Epidermal Barrier Function.
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Jimenez, Lesle M, Oliver, Mary A, Keyloun, John W, Moffatt, Lauren T, Travis, Taryn E, Shupp, Jeffrey W, and Carney, Bonnie C
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HYPERTROPHIC scars ,LASER therapy ,LASERS ,GENE expression ,PROTEIN expression - Abstract
Mechanisms and timing of hypertrophic scar (HTS) improvement with laser therapy are incompletely understood. Epidermal keratinocytes influence HTS through paracrine signaling, yet they are understudied compared to fibroblasts. It was hypothesized that fractional ablative CO
2 laser scar revision (FLSR) would change the fibrotic histoarchitecture of the epidermis in HTS. Duroc pigs (n = 4 FLSR and n = 4 controls) were injured and allowed to form HTS. HTS and normal skin (NS) were assessed weekly by noninvasive skin probes measuring trans-epidermal water loss (TEWL) and biopsy collection. There were 4 weekly FLSR treatments. Immediate laser treatment began on day 49 postinjury (just after re-epithelialization), and early treatment began on day 77 postinjury. Punch biopsies from NS and HTS were processed and stained with H&E. Epidermal thickness and rete ridge ratios (RRR) were measured. Gene and protein expression of involucrin (IVL) and filaggrin (FIL) were examined through qRT-PCR and immunofluorescent (IF) staining. After treatment, peeling sheets of stratum corneum were apparent which were not present in the controls. TEWL was increased in HTS vs NS at day 49, indicating decreased barrier function (P =.05). In the immediate group, TEWL was significantly decreased at week 4 (P <.05). The early group was not significantly different from NS at the prelaser timepoint. After four sessions, the epidermal thickness was significantly increased in treated scars in both FLSR groups (immediate: P <.01 and early: P <.001, n = 8 scars). Early intervention significantly increased RRR (P <.05), and immediate treatment trended toward an increase. There was no increase in either epidermal thickness or RRR in the controls. In the immediate intervention group, there was increased IVL gene expression in HTS vs NS that decreased after FLSR. Eight scars had upregulated gene expression of IVL vs NS levels pretreatment (fold change [FC] > 1.5) compared to four scars at week 4. This was confirmed by IF where IVL staining decreased after FLSR. FIL gene expression trended towards a decrease in both interventions after treatment. Changes in epidermal HTS histoarchitecture and expression levels of epidermal differentiation markers were induced by FLSR. The timing of laser intervention contributed to differences in TEWL, epidermal thickness, and RRR. These data shed light on the putative mechanisms of improvement seen after FLSR treatment. Resolution of timing must be further explored to enhance efficacy. An increased understanding of the difference between the natural history of HTS improvement over time and interventional-induced changes will be critical to justifying the continued approved usage of this treatment. [ABSTRACT FROM AUTHOR]- Published
- 2023
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9. The Potential of Arterial Pulse Wave Analysis in Burn Resuscitation: A Pilot In Vivo Study.
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ArabiDarrehDor, Ghazal, Kao, Yi-Ming, Oliver, Mary A, Parajuli, Babita, Carney, Bonnie C, Keyloun, John W, Moffatt, Lauren T, Shupp, Jeffrey W, Hahn, Jin-Oh, and Burmeister, David M
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PULSE wave analysis ,RESUSCITATION ,SYSTOLIC blood pressure ,ARTIFICIAL respiration ,HEMODYNAMIC monitoring - Abstract
While urinary output (UOP) remains the primary endpoint for titration of intravenous fluid resuscitation, it is an insufficient indicator of fluid responsiveness. Although advanced hemodynamic monitoring (including arterial pulse wave analysis [PWA]) is of recent interest, the validity of PWA-derived indices in burn resuscitation extremes has not been established. The goal of this paper is to test the hypothesis that PWA-derived cardiac output (CO) and stroke volume (SV) indices as well as pulse pressure variation (PPV) and systolic pressure variation (SPV) can play a complementary role to UOP in burn resuscitation. Swine were instrumented with a Swan-Ganz catheter for reference CO and underwent a 40% TBSA burns with varying resuscitation paradigms, and were monitored for 24 hours in an ICU setting under mechanical ventilation. The longitudinal changes in PWA-derived indices were investigated, and resuscitation adequacy was compared as determined by UOP vs PWA indices. The results indicated that PWA-derived indices exhibited trends consistent with reference CO and SV measurements: CO and SV indices were proportional to reference CO and SV, respectively (CO: postcalibration limits of agreement [LoA] = ±24.7 [ml/min/kg], SV: postcalibration LoA = ±0.30 [ml/kg]) while PPV and SPV were inversely proportional to reference SV (PPV: postcalibration LoA = ±0.32 [ml/kg], SPV: postcalibration LoA = ±0.31 [ml/kg]). The results also indicated that PWA-derived indices exhibited notable discrepancies from UOP in determining adequate burn resuscitation. Hence, it was concluded that the PWA-derived indices may have complementary value to UOP in assessing and guiding burn resuscitation. [ABSTRACT FROM AUTHOR]
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- 2023
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10. Proceedings of the 2021 American Burn Association State and Future of Burn Science Meeting.
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Group, The 2021 American Burn Association State and Future of Burn Science Working, Moffatt, Lauren T, and 2021 American Burn Association State and Future of Burn Science Working Group
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BURNS & scalds - Abstract
Periodically, the American Burn Association (ABA) has convened a State of the Science meeting on various topics representing multiple disciplines within burn care and research. In 2021 at the request of the ABA President, meeting development was guided by the ABA's Burn Science Advisory Panel (BSAP) and a subgroup of meeting chairs. The goal of the meeting was to produce both an evaluation of the current literature and ongoing studies, and to produce a research agenda and/or define subject matter-relevant next steps to advance the field(s). Members of the BSAP defined the topics to be addressed and subsequently solicited for nominations of expert speakers and topic leaders from the ABA's Research Committee. Current background literature for each topic was compiled by the meeting chairs and the library then enhanced by the invited topic and breakout discussion leaders. The meeting was held in New Orleans, LA on November 2nd and 3rd and was formatted to allow for 12 different topics, each with two subtopics, to be addressed. Topic leaders provided a brief overview of each topic to approximately 100 attendees, followed by expert-lead breakout sessions for each topic that allowed for focused discussion among subject matter experts and interested participants. The breakout and topic group leaders worked with the participants to determine research needs and associated next steps including white papers, reviews and in some cases collaborative grant proposals. Here, summaries from each topic area will be presented to highlight the main foci of discussion and associated conclusions. [ABSTRACT FROM AUTHOR]
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- 2022
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11. Angiogenic gene characterization and vessel permeability of dermal microvascular endothelial cells isolated from burn hypertrophic scar.
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Molina, Esteban A., Hartmann, Brandon, Oliver, Mary A., Kirkpatrick, Liam D., Keyloun, John W., Moffatt, Lauren T., Shupp, Jeffrey W., Travis, Taryn E., and Carney, Bonnie C.
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HYPERTROPHIC scars ,ENDOTHELIAL cells ,PERMEABILITY ,GENES ,ENDOTHELIUM diseases ,SCARS - Abstract
Hypertrophic scar (HTS) formation is a common challenge for patients after burn injury. Dermal microvascular endothelial cells (DMVECs) are an understudied cell type in HTS. An increase in angiogenesis and microvessel density can be observed in HTS. Endothelial dysfunction may play a role in scar development. This study aims to generate a functional and expression profile of HTS DMVECs. We hypothesize that transcript and protein-level responses in HTS DMVECs differ from those in normal skin (NS). HTSs were created in red Duroc pigs. DMVECs were isolated using magnetic-activated cell sorting with ulex europaeus agglutinin 1 (UEA-1) lectin. Separate transwell inserts were used to form monolayers of HTS DMVECs and NS DMVECs. Cell injury was induced and permeability was assessed. Gene expression in HTS DMVECS versus NS DMVECs was measured. Select differentially expressed genes were further investigated. HTS had an increased area density of dermal microvasculature compared to NS. HTS DMVECs were 17.59% less permeable than normal DMVECs (p < 0.05). After injury, NS DMVECs were 28.4% and HTS DMVECs were 18.8% more permeable than uninjured controls (28.4 ± 4.8 vs 18.8 ± 2.8; p = 0.11). PCR array identified 31 differentially expressed genes between HTS and NS DMVECs, of which 10 were upregulated and 21 were downregulated. qRT-PCR and ELISA studies were in accordance with the array. DMVECs expressed a mixed profile of factors that can contribute to and inhibit scar formation. HTS DMVECs have both a discordant response to cellular insults and baseline differences in function, supporting their proposed role in scar pathology. Further investigation of DMVECs is warranted to elucidate their contribution to HTS pathogenesis. [ABSTRACT FROM AUTHOR]
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- 2022
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12. Comparison of Transcriptional Signatures of Three Staphylococcal Superantigenic Toxins in Human Melanocytes.
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Chakraborty, Nabarun, Srinivasan, Seshamalini, Yang, Ruoting, Miller, Stacy-Ann, Gautam, Aarti, Detwiler, Leanne J., Carney, Bonnie C., Alkhalil, Abdulnaser, Moffatt, Lauren T., Jett, Marti, Shupp, Jeffrey W., and Hammamieh, Rasha
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MELANOCYTES ,TOXINS ,TOXIC shock syndrome ,SUPERANTIGENS ,ENTEROTOXINS - Abstract
Staphylococcus aureus, a gram-positive bacterium, causes toxic shock through the production of superantigenic toxins (sAgs) known as Staphylococcal enterotoxins (SE), serotypes A-J (SEA, SEB, etc.), and toxic shock syndrome toxin-1 (TSST-1). The chronology of host transcriptomic events that characterizes the response to the pathogenesis of superantigenic toxicity remains uncertain. The focus of this study was to elucidate time-resolved host responses to three toxins of the superantigenic family, namely SEA, SEB, and TSST-1. Due to the evolving critical role of melanocytes in the host's immune response against environmental harmful elements, we investigated herein the transcriptomic responses of melanocytes after treatment with 200 ng/mL of SEA, SEB, or TSST-1 for 0.5, 2, 6, 12, 24, or 48 h. Functional analysis indicated that each of these three toxins induced a specific transcriptional pattern. In particular, the time-resolved transcriptional modulations due to SEB exposure were very distinct from those induced by SEA and TSST-1. The three superantigens share some similarities in the mechanisms underlying apoptosis, innate immunity, and other biological processes. Superantigen-specific signatures were determined for the functional dynamics related to necrosis, cytokine production, and acute-phase response. These differentially regulated networks can be targeted for therapeutic intervention and marked as the distinguishing factors for the three sAgs. [ABSTRACT FROM AUTHOR]
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- 2022
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13. Compounded Cerium Nitrate-Silver Sulfadiazine Cream is Safe and Effective for the Treatment of Burn Wounds: A Burn Center's 4-Year Experience.
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Reese, Adam D, Keyloun, John W, Garg, Gaurav, McLawhorn, Melissa M, Moffatt, Lauren T, Travis, Taryn E, Johnson, Laura S, and Shupp, Jeffrey W
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Wound infections and sepsis are significant causes of morbidity after burn injury and can be alleviated by early excision and grafting. In situations that preclude early surgery, topical agents allow for a safer delay. Cerium nitrate compounded with silver sulfadiazine (Ce-SSD) is a burn cream that provides broad antibacterial activity, forms a temporary barrier, and promotes re-epithelialization. Methemoglobinemia is a rare, but oft-cited, systemic complication of Ce-SSD. In this retrospective review, 157 patients treated with Ce-SSD between July 2014 and July 2018 were identified, and the monitoring protocol for methemoglobinemia during Ce-SSD treatment was evaluated. The median age was 59 years (interquartile range [IQR], 47-70.5 years), with TBSA of 8.5% (IQR, 3-27), adjusted Baux score of 76 (IQR, 59-94), and inhalation injury present in 9.9% of patients. Primary endpoints included incidence of symptomatic and asymptomatic methemoglobinemia. Of the 9.6% (n = 15) of patients with methemoglobinemia, 73.3% (n = 11) had maximum methemoglobin levels ≥72 hours from the time of the first application. One patient developed clinically significant methemoglobinemia. Patients with TBSA ≥20% were more likely to develop methemoglobinemia (odds ratio 9.318, 95% confidence interval 2.078-65.73, P = .0078); however, neither Ce-SSD doses nor days of exposure were significant predictors. Ce-SSD application to temporize burn wounds until excision and grafting is safe, effective, and, in asymptomatic patients with TBSA <20%, can be used without serial blood gas monitoring. Vigilant monitoring for symptoms should be performed in patients with TBSA ≥20%, but routine blood gases are not necessary. [ABSTRACT FROM AUTHOR]
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- 2022
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14. Early Transcriptomic Response to Burn Injury: Severe Burns Are Associated With Immune Pathway Shutdown.
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Keyloun, John W, Campbell, Ross, Carney, Bonnie C, Yang, Ruoting, Miller, Stacy-Ann, Detwiler, Leanne, Gautam, Aarti, Moffatt, Lauren T, Hammamieh, Rasha, Jett, Marti, Shupp, Jeffrey W, group, SYSCOT study, and SYSCOT study group
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BURN patients ,BURNS & scalds ,INFLAMMATION ,RNA ,SEVERITY of illness index ,GENE expression profiling ,IMMUNITY ,BIOCHIPS ,DESCRIPTIVE statistics ,LONGITUDINAL method - Abstract
Burn injury induces a systemic hyperinflammatory response with detrimental side effects. Studies have described the biochemical changes induced by severe burns, but the transcriptome response is not well characterized. The goal of this work is to characterize the blood transcriptome after burn injury. Burn patients presenting to a regional center between 2012 and 2017 were prospectively enrolled. Blood was collected on admission and at predetermined time points (hours 2, 4, 8, 12, and 24). RNA was isolated and transcript levels were measured with a gene expression microarray. To identify differentially regulated genes (false-discovery rate ≤0.1) by burn injury severity, patients were grouped by TBSA above or below 20% and statistically enriched pathways were identified. Sixty-eight patients were analyzed, most patients were male with a median age of 41 (interquartile range, 30.5-58.5) years, and TBSA of 20% (11%-34%). Thirty-five patients had % TBSA injury ≥20%, and this group experienced greater mortality (26% vs 3%, P = .008). Comparative analysis of genes from patients with ≥20% TBSA revealed 1505, 613, 380, 63, 1357, and 954 differentially expressed genes at hours 0, 2, 4, 8, 12, and 24, respectively. Pathway analysis revealed an initial up-regulation in several immune/inflammatory pathways within the ≥20% TBSA groups followed by shutdown. Severe burn injury is associated with an early proinflammatory immune response followed by shutdown of these pathways. Examination of the immunoinflammatory response to burn injury through differential gene regulation and associated immune pathways by injury severity may identify mechanistic targets for future intervention. [ABSTRACT FROM AUTHOR]
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- 2022
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15. Inhalation Injury Is Associated With Endotheliopathy and Abnormal Fibrinolytic Phenotypes in Burn Patients: A Cohort Study.
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Keyloun, John W, Le, Tuan D, Brummel-Ziedins, Kathleen E, Mclawhorn, Melissa M, Bravo, Maria C, Orfeo, Thomas, Johnson, Laura S, Moffatt, Lauren T, Pusateri, Anthony E, Shupp, Jeffrey W, Group, SYSCOT Study, and SYSCOT Study Group
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DISSEMINATED intravascular coagulation ,EVALUATION of medical care ,BURN patients ,ENDOTHELIUM ,MORTALITY ,SMOKE inhalation injuries ,RETROSPECTIVE studies ,BLOOD collection ,THROMBELASTOGRAPHY ,HEALTH outcome assessment ,MANN Whitney U Test ,FISHER exact test ,FIBRINOLYSIS ,ENZYME-linked immunosorbent assay ,CHI-squared test ,DESCRIPTIVE statistics ,PHENOTYPES ,LONGITUDINAL method ,DISEASE risk factors ,DISEASE complications - Abstract
Burn injury is associated with endothelial dysfunction and coagulopathy and concomitant inhalation injury (IHI) increases morbidity and mortality. The aim of this work is to identify associations between IHI, coagulation homeostasis, vascular endothelium, and clinical outcomes in burn patients. One hundred and twelve patients presenting to a regional burn center were included in this retrospective cohort study. Whole blood was collected at set intervals from admission through 24 hours and underwent viscoelastic assay with rapid thromboelastography (rTEG). Syndecan-1 (SDC-1) on admission was quantified by ELISA. Patients were grouped by the presence (n = 28) or absence (n = 84) of concomitant IHI and rTEG parameters, fibrinolytic phenotypes, SDC-1, and clinical outcomes were compared. Of the 112 thermally injured patients, 28 (25%) had IHI. Most patients were male (68.8%) with a median age of 40 (interquartile range, 29-57) years. Patients with IHI had higher overall mortality (42.68% vs 8.3%; P < .0001). rTEG LY30 was lower in patients with IHI at hours 4 and 12 (P < .05). There was a pattern of increased abnormal fibrinolytic phenotypes among IHI patients. There was a greater proportion of IHI patients with endotheliopathy (SDC-1 > 34 ng/ml) (64.7% vs 26.4%; P = .008). There was a pattern of increased mortality among patients with IHI and endotheliopathy (0% vs 72.7%; P = .004). Significant differences between patients with and without IHI were found in measures assessing fibrinolytic potential and endotheliopathy. Mortality was associated with abnormal fibrinolysis, endotheliopathy, and IHI. However, the extent to which IHI-associated dysfunction is independent of TBSA burn size remains to be elucidated. [ABSTRACT FROM AUTHOR]
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- 2022
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16. Transcriptomics of Wet Skin Biopsies Predict Early Radiation-Induced Hematological Damage in a Mouse Model.
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Alkhalil, Abdulnaser, Clifford, John, Miller, Stacy Ann, Gautam, Aarti, Jett, Marti, Hammamieh, Rasha, Moffatt, Lauren T., and Shupp, Jeffrey W.
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The lack of an easy and fast radiation-exposure testing method with a dosimetric ability complicates triage and treatment in response to a nuclear detonation, radioactive material release, or clandestine exposure. The potential of transcriptomics in radiation diagnosis and prognosis were assessed here using wet skin (blood/skin) biopsies obtained at hour 2 and days 4, 7, 21, and 28 from a mouse radiation model. Analysis of significantly differentially transcribed genes (SDTG; p ≤ 0.05 and FC ≥ 2) during the first post-exposure week identified the glycoprotein 6 (GP-VI) signaling, the dendritic cell maturation, and the intrinsic prothrombin activation pathways as the top modulated pathways with stable inactivation after lethal exposures (20 Gy) and intermittent activation after sublethal (1, 3, 6 Gy) exposure time points (TPs). Interestingly, these pathways were inactivated in the late TPs after sublethal exposure in concordance with a delayed deleterious effect. Modulated transcription of a variety of collagen types, laminin, and peptidase genes underlay the modulated functions of these hematologically important pathways. Several other SDTGs related to platelet and leukocyte development and functions were identified. These results outlined genetic determinants that were crucial to clinically documented radiation-induced hematological and skin damage with potential countermeasure applications. [ABSTRACT FROM AUTHOR]
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- 2022
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17. In‐depth examination of hyperproliferative healing in two breeds of Sus scrofa domesticus commonly used for research.
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Funkhouser, Colton H., Kirkpatrick, Liam D., Smith, Robert D., Moffatt, Lauren T., Shupp, Jeffrey W., and Carney, Bonnie C.
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- 2021
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18. Review of the Terminology Describing Ionizing Radiation-Induced Skin Injury: A Case for Standardization.
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Burnett, Luke R., Hughes, Ryan T., Rejeski, Alexis F., Moffatt, Lauren T., Shupp, Jeffrey W., Christy, Robert J., and Winkfield, Karen M.
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SKIN injuries ,RADIODERMATITIS ,RADIATION injuries ,MEDICAL personnel ,WOUND care ,SKIN - Abstract
Ionizing radiation causes injury to the skin that produces a complex clinical presentation that is managed by various paradigms without clear standards. The situation is further complicated by the fact that clinicians and researchers often use different terms and billing codes to describe the spectrum of cutaneous injury. There is, however, general agreement between the two most commonly-used diagnostic scales, the Radiation Therapy Oncology Group and the Common Terminology Criteria for Adverse Events, and in their use to describe skin injury following radiation therapy. These scales are typically used by radiation oncologists to quantify radiation dermatitis, a component of the radiation-related disorders of the skin and subcutaneous tissue family of diagnoses. In rare cases, patients with severe injury may require treatment by wound care or burn specialists, in which case the disease is described as a "radiation burn" and coded as a burn or corrosion. Further compounding the issue, most US government agencies use the term Cutaneous Radiation Injury to indicate skin damage resulting from large, whole-body exposures. In contrast, the US Food and Drug Administration approves products for radiation dermatitis or "burns caused by radiation oncology procedures." A review of the literature and comparison of clinical presentations shows that each of these terms represents a similar injury, and can be used interchangeably. Herein we provide a comparative review of the commonly used terminology for radiation-induced skin injury. Further, we recommend standardization across clinicians, providers, and researchers involved in the diagnosis, care, and investigation of radiation-induced skin injury. This will facilitate collaboration and broader inclusion criteria for grant-research and clinical trials and will assist in assessing therapeutic options particularly relevant to patient skin pigmentation response differences. [ABSTRACT FROM AUTHOR]
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- 2021
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19. Examining the effect of wound cleansing on the microbiome of venous stasis ulcers.
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Ernlund, Amanda W., Moffatt, Lauren T., Timm, Collin M., Zudock, Kristina K., Howser, Craig W., Blount, Kianna M., Alkhalil, Abdulnaser, Shupp, Jeffrey W., and Karig, David K.
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CHRONIC wounds & injuries ,SEQUENCE analysis ,PROTEUS (Bacteria) ,DEBRIDEMENT ,CULTURES (Biology) ,HUMAN microbiota ,LEG ulcers ,PSEUDOMONAS ,WOUND care - Abstract
Common treatment for venous leg wounds includes topical wound dressings with compression. At each dressing change, wounds are debrided and washed; however, the effect of the washing procedure on the wound microbiome has not been studied. We hypothesized that wound washing may alter the wound microbiome. To characterize microbiome changes with respect to wound washing, swabs from 11 patients with chronic wounds were sampled before and after washing, and patient microbiomes were characterized using 16S rRNA sequencing and culturing. Microbiomes across patient samples prior to washing were typically polymicrobial but varied in the number and type of bacterial genera present. Proteus and Pseudomonas were the dominant genera in the study. We found that washing does not consistently change microbiome diversity but does cause consistent changes in microbiome composition. Specifically, washing caused a decrease in the relative abundance of the most highly represented genera in each patient cluster. The finding that venous leg ulcer wound washing, a standard of care therapy, can induce changes in the wound microbiome is novel and could be potentially informative for future guided therapy strategies. [ABSTRACT FROM AUTHOR]
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- 2021
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20. CIRCULATING SYNDECAN-1 AND TISSUE FACTOR PATHWAY INHIBITOR, BIOMARKERS OF ENDOTHELIAL DYSFUNCTION, PREDICT MORTALITY IN BURN PATIENTS.
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Keyloun, John W., Le, Tuan D., Pusateri, Anthony E., Ball, Robert L., Carney, Bonnie C., Orfeo, Thomas, Brummel-Ziedins, Kathleen E., Bravo, Maria C., McLawhorn, Melissa M., Moffatt, Lauren T., and Shupp, Jeffrey W.
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- 2021
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21. Cutaneous Thermal Injury Modulates Blood and Skin Metabolomes Differently in a Murine Model.
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Alkhalil, Abdulnaser, Ball, Robert L, Garg, Gaurav, Day, Anna, Carney, Bonnie C, Kumar, Raina, Hammamieh, Rasha, Moffatt, Lauren T, and Shupp, Jeffrey W
- Subjects
METABOLOMICS ,PENTOSE phosphate pathway ,PHOSPHATE metabolism ,INOSITOL phosphates ,PATHOLOGICAL physiology - Abstract
As the field of metabolomics develops further, investigations of how the metabolome is affected following thermal injury may be helpful to inform diagnostics and guide treatments. In this study, changes to the metabolome were tested and validated in a murine burn injury model. After a 30% total body surface scald injury or sham procedure sera and skin biopsies were collected at 1, 2, 6, or 24 hr. Burn-specific changes in the metabolome were detected compared to sham animals. The sera metabolome exhibited a more rapid response to burn injury than that of the skin and it peaked more proximal to injury (6 vs 24 hr). Progression of metabolic response in the skin was less synchronous and showed a higher overlap of the significantly modified metabolites (SMMs) among tested time-points. Top affected pathways identified by SMMs of skin included inositol phosphate metabolism, ascorbate and alderate metabolism, caffeine metabolism, and the pentose phosphate pathway. Future research is warranted in human and larger animal models to further elucidate the role of metabolomic perturbations and the pathophysiology following burn injury. [ABSTRACT FROM AUTHOR]
- Published
- 2021
- Full Text
- View/download PDF
22. Institutional Experience Using a Treatment Algorithm for Electrical Injury.
- Author
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Nisar, Saira, Keyloun, John W, Kolachana, Sindhura, McLawhorn, Melissa M, Moffatt, Lauren T, Travis, Taryn E, Shupp, Jeffrey W, and Johnson, Laura S
- Subjects
ELECTRICAL injuries ,MEDICAL care costs ,LENGTH of stay in hospitals ,CREATINE kinase ,BURN care units ,HOSPITAL mortality ,INTENSIVE care units ,MEDICAL triage ,PATIENT readmissions ,RETROSPECTIVE studies ,ELECTRICAL burns ,BIOTELEMETRY ,ALGORITHMS - Abstract
Electrical injury has low incidence but is associated with high morbidity and mortality. Variability in diagnosis and management among clinicians can lead to unnecessary testing. This study examines the utility of an electrical injury treatment algorithm by comparing the incidence of testing done on a cohort of patients before and after implementation. Demographics, injury characteristics, and treatment information were collected for patients arriving to a regional burn center with the diagnosis of electrical injury from January 2013 to September 2018. Results were compared for patients admitted before and after the implementation of an electrical injury treatment algorithm in July 2015. There were 56 patients in the pre-algorithm cohort and 38 in the post-algorithm cohort who were of similar demographics. The proportion of creatine kinase (82% vs 47%, P < .0006), troponin (79% vs 34%, P < .0001), and urinary myoglobin (80% vs 45%, P < .0007) testing in the pre-algorithm cohort was significantly higher compared to post-algorithm cohort. There were more days of telemetry monitoring (median [IQR], 1 [1-5] vs 1 [1-1] days, P = .009) and greater ICU length of stays (4 [1-5] vs 1 [1-1] days, P = .009), prior to algorithm implementation. There were no significant differences in total hospital lengths of stay, incidence of ICU admissions, in-hospital mortality, or 30-day readmissions. This study demonstrates an electrical injury evaluation and treatment algorithm suggests a mode of triage to cardiac monitoring and hospital admission where necessary. Use of this algorithm allowed for reduction in testing and health care costs without increasing mortality or readmission rates. [ABSTRACT FROM AUTHOR]
- Published
- 2021
- Full Text
- View/download PDF
23. Hypopigmented burn hypertrophic scar contains melanocytes that can be signaled to re-pigment by synthetic alpha-melanocyte stimulating hormone in vitro.
- Author
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Carney, Bonnie C., Travis, Taryn E., Moffatt, Lauren T., Johnson, Laura S., McLawhorn, Melissa M., Simbulan-Rosenthal, Cynthia M., Rosenthal, Dean S., and Shupp, Jeffrey W.
- Subjects
HYPERTROPHIC scars ,MELANOCYTES ,MELANINS ,GENES ,STAINS & staining (Microscopy) ,PHENOTYPES ,GENE expression - Abstract
There are limited treatments for dyschromia in burn hypertrophic scars (HTSs). Initial work in Duroc pig models showed that regions of scar that are light or dark have equal numbers of melanocytes. This study aims to confirm melanocyte presence in regions of hypo- and hyper-pigmentation in an animal model and patient samples. In a Duroc pig model, melanocyte presence was confirmed using en face staining. Patients with dyschromic HTSs had demographic, injury details, and melanin indices collected. Punch biopsies were taken of regions of hyper-, hypo-, or normally pigmented scar and skin. Biopsies were processed to obtain epidermal sheets (ESs). A subset of ESs were en face stained with melanocyte marker, S100β. Melanocytes were isolated from a different subset. Melanocytes were treated with NDP α-MSH, a pigmentation stimulator. mRNA was isolated from cells, and was used to evaluate gene expression of melanin-synthetic genes. In patient and pig scars, regions of hyper-, hypo-, and normal pigmentation had significantly different melanin indices. S100β en face staining showed that regions of hyper- and hypo-pigmentation contained the same number of melanocytes, but these cells had different dendricity/activity. Treatment of hypo-pigmented melanocytes with NDP α-MSH produced melanin by microscopy. Melanin-synthetic genes were upregulated in treated cells over controls. While traditionally it may be thought that hypopigmented regions of burn HTS display this phenotype because of the absence of pigment-producing cells, these data show that inactive melanocytes are present in these scar regions. By treating with a pigment stimulator, cells can be induced to re-pigment. [ABSTRACT FROM AUTHOR]
- Published
- 2021
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24. An Assessment of Research Priorities to Dampen the Pendulum Swing of Burn Resuscitation.
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Burmeister, David M, Smith, Susan L, Muthumalaiappan, Kuzhali, Hill, David M, Moffatt, Lauren T, Carlson, Deborah L, Kubasiak, John C, Chung, Kevin K, Wade, Charles E, Cancio, Leopoldo C, and Shupp, Jeffrey W
- Subjects
THERMAL shock ,RESUSCITATION ,BODY surface area ,TREATMENT for burns & scalds ,EXPERIMENTAL design ,TRAUMATIC shock (Pathology) ,RESEARCH ,RESEARCH methodology ,EVIDENCE-based medicine ,MULTIPLE organ failure ,MEDICAL cooperation ,EVALUATION research ,COMPARATIVE studies ,CRITICAL care medicine ,MEDICAL societies ,STANDARDS - Abstract
On June 17 to 18, 2019, the American Burn Association, in conjunction with Underwriters Laboratories, convened a group of experts on burn resuscitation in Washington, DC. The goal of the meeting was to identify and discuss novel research and strategies to optimize the process of burn resuscitation. Patients who sustain a large thermal injury (involving >20% of the total body surface area [TBSA]) face a sequence of challenges, beginning with burn shock. Over the last century, research has helped elucidate much of the underlying pathophysiology of burn shock, which places multiple organ systems at risk of damage or dysfunction. These studies advanced the understanding of the need for fluids for resuscitation. The resultant practice of judicious and timely infusion of crystalloids has improved mortality after major thermal injury. However, much remains unclear about how to further improve and customize resuscitation practice to limit the morbidities associated with edema and volume overload. Herein, we review the history and pathophysiology of shock following thermal injury, and propose some of the priorities for resuscitation research. Recommendations include: studying the utility of alternative endpoints to resuscitation, reexamining plasma as a primary or adjunctive resuscitation fluid, and applying information about inflammation and endotheliopathy to target the underlying causes of burn shock. Undoubtedly, these future research efforts will require a concerted effort from the burn and research communities. [ABSTRACT FROM AUTHOR]
- Published
- 2021
- Full Text
- View/download PDF
25. Coming to Consensus: What Defines Deep Partial Thickness Burn Injuries in Porcine Models?
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Gibson, Angela L F, Carney, Bonnie C, Cuttle, Leila, Andrews, Christine J, Kowalczewski, Christine J, Liu, Aiping, Powell, Heather M, Stone, Randolph, Supp, Dorothy M, Singer, Adam J, Shupp, Jeffrey W, Stalter, Lily, Moffatt, Lauren T, and Lily, Stalter
- Subjects
BURNS & scalds ,SCORING rubrics ,STAINS & staining (Microscopy) ,ANIMAL models in research ,CHEMICAL burns ,BIOLOGICAL models ,RESEARCH ,ANIMAL experimentation ,RESEARCH methodology ,SWINE ,MEDICAL cooperation ,EVALUATION research ,COMPARATIVE studies - Abstract
Deep partial thickness burns are clinically prevalent and difficult to diagnose. In order to develop methods to assess burn depth and therapies to treat deep partial thickness burns, reliable, accurate animal models are needed. The variety of animal models in the literature and the lack of precise details reported for the experimental procedures make comparison of research between investigators challenging and ultimately affect translation to patients. They sought to compare deep partial thickness porcine burn models from five well-established laboratories. In doing so, they uncovered a lack of consistency in approaches to the evaluation of burn injury depth that was present within and among various models. They then used an iterative process to develop a scoring rubric with an educational component to facilitate burn injury depth evaluation that improved reliability of the scoring. Using the developed rubric to re-score the five burn models, they found that all models created a deep partial thickness injury and that agreement about specific characteristics identified on histological staining was improved. Finally, they present consensus statements on the evaluation and interpretation of the microanatomy of deep partial thickness burns in pigs. [ABSTRACT FROM AUTHOR]
- Published
- 2021
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- View/download PDF
26. Galectin‐1 production is elevated in hypertrophic scar.
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Kirkpatrick, Liam D., Shupp, Jeffrey W., Smith, Robert D., Alkhalil, Abdulnaser, Moffatt, Lauren T., and Carney, Bonnie C.
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ANIMAL experimentation ,HYPERTROPHIC scars - Abstract
Upon healing, burn wounds often leave hypertrophic scars (HTSs) marked by excess collagen deposition, dermal and epidermal thickening, hypervascularity, and an increased density of fibroblasts. The Galectins, a family of lectins with a conserved carbohydrate recognition domain, function intracellularly and extracellularly to mediate a multitude of biological processes including inflammatory responses, angiogenesis, cell migration and differentiation, and cell‐ECM adhesion. Galectin‐1 (Gal‐1) has been associated with several fibrotic diseases and can induce keratinocyte and fibroblast proliferation, migration, and differentiation into fibroproliferative myofibroblasts. In this study, Gal‐1 expression was assessed in human and porcine HTS. In a microarray, galectins 1, 4, and 12 were upregulated in pig HTS compared to normal skin (fold change = +3.58, +6.11, and +3.03, FDR <0.01). Confirmatory qRT‐PCR demonstrated significant upregulation of Galectin‐1 (LGALS1) transcription in HTS in both human and porcine tissues (fold change = +7.78 and +7.90, P <.05). In pig HTS, this upregulation was maintained throughout scar development and remodeling. Immunofluorescent staining of Gal‐1 in human and porcine HTS showed significantly increased fluorescence (202.5 ± 58.2 vs 35.2 ± 21.0, P <.05 and 276.1 ± 12.7 vs 69.7 ± 25.9, P <.01) compared to normal skin and co‐localization with smooth muscle actin‐expressing myofibroblasts. A strong positive correlation (R =.948) was observed between LGALS1 and Collagen type 1 alpha 1 mRNA expression. Gal‐1 is overexpressed in HTS at the mRNA and protein levels and may have a role in the development of scar phenotypes due to fibroblast over‐proliferation, collagen secretion, and dermal thickening. The role of galectins shows promise for future study and may lead to the development of a pharmacotherapy for treatment of HTS. [ABSTRACT FROM AUTHOR]
- Published
- 2021
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- View/download PDF
27. BURN-INDUCED COAGULOPATHIES: A COMPREHENSIVE REVIEW.
- Author
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Ball, Robert L., Keyloun, John W., Brummel-Ziedins, Kathleen, Orfeo, Thomas, Palmieri, Tina L., Johnson, Laura S., Moffatt, Lauren T., Pusateri, Anthony E., and Shupp, Jeffrey W.
- Published
- 2020
- Full Text
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28. Blood RNA Integrity is a Direct and Simple Reporter of Radiation Exposure and Prognosis: A Pilot Study.
- Author
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Alkhalil, Abdulnaser, Clifford, John. L., Ball, Robert, Day, Anna, Chan, Rosanna, Carney, Bonnie C., Miller, Stacy Ann, Campbell, Ross, Kumar, Raina, Gautam, Aarti, Hammamieh, Rasha, Moffatt, Lauren T., and Shupp, Jeffrey W.
- Subjects
RADIATION exposure ,RNA ,IONIZING radiation ,BODY surface area ,MEDICAL personnel ,PILOT projects - Abstract
In the event of a mass casualty radiation scenario, rapid assessment of patients' health and triage is required for optimal resource utilization. Identifying the level and extent of exposure as well as prioritization of care is extremely challenging under such disaster conditions. Blood-based biomarkers, such as RNA integrity numbers (RIN), could help healthcare personnel quickly and efficiently determine the extent and effect of multiple injuries on patients' health. Evaluation of the effect of different radiation doses, alone or in combination with burn injury, on total RNA integrity over multiple time points was performed. Total RNA integrity was tallied in blood samples for potential application as a marker of radiation exposure and survival. Groups of aged mice (3–6 mice/group, 13–18 months old) received 0.5, 1, 5, 10 or 20 Gy ionizing radiation. Two additional mouse groups received low-dose irradiation (0.5 or 1 Gy) with a 15% total body surface area (TBSA) burn injury. Animals were euthanized at 2 or 12 h and at day 1, 2, 3, 7 or 14 postirradiation, or when injury-mediated mortality occurred. Total RNA was isolated from blood. The quality of RNA was evaluated and RNA RIN were obtained. Analysis of RIN indicated that blood showed the clearest radiation effect. There was a time- and radiation-dose-dependent reduction in RIN that was first detectable at 12 h postirradiation for all doses in animals receiving irradiation alone. This effect was reversible in lower-dose groups (i.e., 0.5, 1 and 5 Gy) that survived to the end of the study (14 days). In contrast, the effect persisted for 10 and 20 Gy groups, which showed suppression of RIN values <4.5 with high mortalities. Radiation doses of 20 Gy were lethal and required euthanasia by day 6. A low RIN (<2.5) at any time point was associated with 100% mortality. Combined radiation-burn injury produced significantly increased mortality such that no dually-injured animals survived beyond day 3, and no radiation dose >1 Gy resulted in survival past day 1. More modest suppression of RIN was observed in the surviving dually challenged mice, and no statistically significant changes were identified in RIN values of burn-only mice at any time point. In this study of an animal model, a proof of concept is presented for a simple and accurate method of assessing radiation dose exposure in blood which potentially predicts lethality. RIN assessment of blood-derived RNA could form the basis for a clinical decision-support tool to guide healthcare providers under the strenuous conditions of a radiation-based mass casualty event. [ABSTRACT FROM AUTHOR]
- Published
- 2020
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- View/download PDF
29. Standards in Biologic Lesions: Cutaneous Thermal Injury and Inhalation Injury Working Group 2018 Meeting Proceedings.
- Author
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Moffatt, Lauren T, Madrzykowski, Daniel, Gibson, Angela L F, Powell, Heather M, Cancio, Leopoldo C, Wade, Charles E, Choudhry, Mashkoor A, Kovacs, Elizabeth J, Finnerty, Celeste C, Majetschak, Matthias, Shupp, Jeffrey W, Group, The Standards in Biologic Lesions Working, and Standards in Biologic Lesions Working Group
- Subjects
INHALATION injuries ,TEAMS in the workplace ,FIRES & the environment ,LABORATORY safety ,TRANSLATIONAL research ,HEMORRHAGIC shock ,TREATMENT for burns & scalds ,RESEARCH ,RESEARCH methodology ,MEDICAL cooperation ,EVALUATION research ,COMPARATIVE studies ,FIRES ,PHENOTYPES - Abstract
On August 27 and 28, 2018, the American Burn Association, in conjunction with Underwriters Laboratories, convened a group of experts on burn and inhalation injury in Washington, DC. The goal of the meeting was to identify and discuss the existing knowledge, data, and modeling gaps related to understanding cutaneous thermal injury and inhalation injury due to exposure from a fire environment, and in addition, address two more areas proposed by the American Burn Association Research Committee that are critical to burn care but may have current translational research gaps (inflammatory response and hypermetabolic response). Representatives from the Underwriters Laboratories Firefighter Safety Research Institute and the Bureau of Alcohol, Tobacco, Firearms and Explosives Fire Research Laboratory presented the state of the science in their fields, highlighting areas that required further investigation and guidance from the burn community. Four areas were discussed by the full 24 participant group and in smaller groups: Basic and Translational Understanding of Inhalation Injury, Thermal Contact and Resulting Injury, Systemic Inflammatory Response and Resuscitation, and Hypermetabolic Response and Healing. A primary finding was the need for validating historic models to develop a set of reliable data on contact time and temperature and resulting injury. The working groups identified common areas of focus across each subtopic, including gaining an understanding of individual response to injury that would allow for precision medicine approaches. Predisposed phenotype in response to insult, the effects of age and sex, and the role of microbiomes could all be studied by employing multi-omic (systems biology) approaches. [ABSTRACT FROM AUTHOR]
- Published
- 2020
- Full Text
- View/download PDF
30. Promoter Methylation Status in Pro-opiomelanocortin Does Not Contribute to Dyspigmentation in Hypertrophic Scar.
- Author
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Carney, Bonnie C, Dougherty, Ryan D, Moffatt, Lauren T, Simbulan-Rosenthal, Cynthia M, Shupp, Jeffrey W, and Rosenthal, Dean S
- Subjects
PROOPIOMELANOCORTIN ,METHYLATION ,MELANOCORTIN receptors ,BIOLOGICAL pigments ,PROTEIN expression ,HYPERTROPHIC scars - Abstract
Burn injuries frequently result in hypertrophic scars (HTSs), specifically when excision and grafting are delayed due to limited resources or patient complications. In patient populations with dark baseline pigmentation, one symptom of HTS that often occurs is dyspigmentation. The mechanism behind dyspigmentation has not been explored, and, as such, prevention and treatment strategies for this morbidity are lacking. The mechanism by which cells make pigment is controlled at the apex of the pathway by pro-opiomelanocortin (POMC), which is cleaved to its products alpha-melanocyte-stimulating hormone (α-MSH) and adrenocorticotropin hormone (ACTH). α-MSH and ACTH secreted by keratinocytes bind to melanocortin 1 receptor (MC1R), expressed on melanocytes, to initiate melanogenesis. POMC protein expression is upregulated in hyperpigmented scar compared to hypopigmented scar by an unknown mechanism in a Duroc pig model of HTS. POMC RNA levels, as well as the POMC gene promoter methylation status were investigated as a possible mechanism. DNA was isolated from biopsies obtained from distinct areas of hyper- or hypopigmented scar and normal skin. DNA was bisulfite-converted, and amplified using two sets of primers to observe methylation patterns in two different CpG islands near the POMC promoter. Amplicons were then sequenced and methylation patterns were evaluated. POMC gene expression was significantly downregulated in hypopigmented scar compared to normal skin, consistent with previously reported protein expression levels. There were significant changes in methylation of the POMC promoter; however, none that would account for the development of hyper- or hypopigmentation. Future work will focus on other areas of POMC transcriptional regulation. [ABSTRACT FROM AUTHOR]
- Published
- 2020
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- View/download PDF
31. Dyspigmented hypertrophic scars: Beyond skin color.
- Author
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Alkhalil, Abdulnaser, Carney, Bonnie C., Travis, Taryn E., Muhie, Seid, Miller, Stacy Ann, Ramella‐Roman, Jessica C., Ghassemi, Pehman, Hammamieh, Rasha, Jett, Marti, Moffatt, Lauren T., and Shupp, Jeffrey W.
- Subjects
HYPERTROPHIC scars ,HUMAN skin color ,MELANOGENESIS ,CELL differentiation ,GENE targeting - Abstract
Although pigment synthesis is well understood, relevant mechanisms of psychologically debilitating dyspigmentation in nascent tissue after cutaneous injuries are still unknown. Here, differences in genomic transcription of hyper‐ and hypopigmented tissue relative to uninjured skin were investigated using a red Duroc swine scar model. Transcription profiles differed based on pigmentation phenotypes with a trend of more upregulation or downregulation in hyper‐ or hypopigmented scars, respectively. Ingenuity Pathway Analysis of significantly modulated genes in both pigmentation phenotypes showed pathways related to redox, metabolic, and inflammatory responses were more present in hypopigmented samples, while those related to stem cell development differentiation were found mainly in hyperpigmented samples. Cell–cell and cell–extracellular matrix interactions and inflammation responses were predicted (z‐score) active in hyperpigmented and inactive in hypopigmented. The proinflammatory high‐mobility group box 1 pathway showed the opposite trend. Analysis of differentially regulated mutually exclusive genes showed an extensive presence of metabolic, proinflammatory, and oxidative stress pathways in hypopigmented scars, while melanin synthesis, glycosaminoglycans biosynthesis, and cell differentiation pathways were predominant in hyperpigmented scar. Several potential therapeutic gene targets have been identified. [ABSTRACT FROM AUTHOR]
- Published
- 2019
- Full Text
- View/download PDF
32. Pigmentation Diathesis of Hypertrophic Scar: An Examination of Known Signaling Pathways to Elucidate the Molecular Pathophysiology of Injury-Related Dyschromia.
- Author
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Carney, Bonnie C, Chen, Jason H, Luker, Jenna N, Alkhalil, Abdulnaser, Jo, Daniel Y, Travis, Taryn E, Moffatt, Lauren T, Simbulan-Rosenthal, Cynthia M, Rosenthal, Dean S, and Shupp, Jeffrey W
- Subjects
HYPERTROPHIC scars ,STEM cell factor ,PATHOLOGICAL physiology ,ANIMAL coloration ,MELANOCORTIN receptors ,CARTILAGE cells - Abstract
Hypertrophic scar (HTS) occurs frequently after burn injury. Treatments for some aspects of scar morbidity exist, however, dyspigmentation treatments are lacking due to limited knowledge about why scars display dyschromic phenotypes. Full thickness wounds were created on duroc pigs that healed to form dyschromic HTS. HTS biopsies and primary cell cultures were then used to study pigmentation signaling. Biopsies of areas of both pigment types were taken for analysis. At the end of the experiment, melanocyte-keratinocyte cocultures were established from areas of differential pigmentation. Heterogeneously dyspigmented scars formed with regions of hyperpigmentation and hypopigmentation. Melanocytes were present in both pigment types measured by S100β quantitative real time-polymerase chain reaction (qRT-PCR) and immunostaining, and visualized by dendritic cell presence in primary cultures. P53 expression was not different between the two pigment types. Hyperpigmented scars had upregulated levels of proopiomelanocortin (POMC), adrenocorticotropic hormone (ACTH), α-melanocyte stimulating hormone (α-MSH), stem cell factor (SCF), and c-KIT and melanocortin 1 receptors (MC1R) compared to hypopigmented regions. Many genes involved in dyspigmentation were differentially regulated by microarray analysis including MITF, TYR, TYRP1, and DCT. MiTF expression was not different upon further exploration, but TYR, TYRP1, and DCT were upregulated in intact biopsies measured by qRT-PCR and confirmed by immunostaining. This is the first work to confirm the presence of melanocytes in hypopigmented scar using qRT-PCR and primary cell culture. An understanding of the initial steps in dyspigmentation signaling, as well as the downstream effects of these signals, will inform treatment options for patients with scars and provide insight to where pharmacotherapy may be directed. [ABSTRACT FROM AUTHOR]
- Published
- 2019
- Full Text
- View/download PDF
33. Further Histological and Cellular Characterization of Hidradenitis Suppurativa in 11 Patients.
- Author
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Nisar, Saira, Roberson, Jeffrey L., Carney, Bonnie C., Alkhalil, Abdulnaser, Moffatt, Lauren T., and Shupp, Jeffrey W.
- Subjects
HIDRADENITIS suppurativa ,VASCULAR endothelial cells ,SURGICAL excision ,CELL anatomy ,SKIN diseases - Abstract
Background: Hidradenitis suppurativa is a chronic inflammatory skin disease, with significant morbidity secondary to its recurrent painful and exudative lesions. Given limited research on the cytoarchitecture of hidradenitis suppurativa, this study describes the microscopic structure and cell surface markers present in hidradenitis suppurativa tissue to better understand the disease and identify potential therapeutic targets. Methods: Skin biopsies of hidradenitis suppurativa lesions from patients who underwent surgical excision (n = 11) were compared with grossly normal-appearing perilesional skin (n = 5) and normal skin biopsies from unaffected individuals (n = 4). Histopathology and epidermal thickness were assessed using hematoxylin and eosin and picrosirius red staining, and CD3, a T-cell marker, and CD31 (PECAM), a vascular endothelial cell marker, were assayed using immunofluorescence. Data were analyzed and compared using analysis of variance and Student’s t test. Results: Histological examination showed that hidradenitis suppurativa samples had a significantly thicker epidermal layer than normal skin (335.23 ± 165.01 μm vs 57.24 ± 18.43 μm, P = .005), extending into and engulfing the dermis. The hidradenitis suppurativa dermis had extensive cellular infiltration and aggregation as well as disorganized collagen. Immunofluorescence analysis revealed that, at the dermal level, hidradenitis suppurativa lesions had a significantly greater quantity of CD3
+ (324.29 ± 139.28 vs 14.93 ±16.32, P < .0001) and CD31+ (322.15 ± 155.46 vs 2.84 ± 5.56, P < .0001) cells/mm2 compared with normal skin samples. Conclusions: Hidradenitis suppurativa lesions have thicker epidermal layers, more dermal cellular infiltrate, and disorganized collagen fibers compared with normal skin. Furthermore, hidradenitis suppurativa dermis has a greater quantity of CD3+ and CD31+ cells than normal skin. [ABSTRACT FROM AUTHOR]- Published
- 2019
34. Photobiomodulation Elicits a Differential Cytokine Response in a Cultured Analogue of Human Skin.
- Author
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Prindeze, Nicholas J., Ardanuy, Jeremy G., Carney, Bonnie C., Moffatt, Lauren T., and Shupp, Jeffrey W.
- Subjects
ENZYME-linked immunosorbent assay ,TISSUE culture ,INTERLEUKIN-6 ,MESSENGER RNA ,WOUND healing ,ELLAGIC acid - Abstract
Background: The study of photobiomodulation in wound healing is encumbered by limited wound study models. The aim of this study was to investigate the efficacy of a 3-dimensional dermal tissue culture model as a cost-saving alternative to conventional photobiomodulation study techniques. Methods: Nine dermal analogue tissue cultures were treated for 2 days with sham or 660-nm wavelength of light at either 1.5 or 3 mW/cm2 of energy. Tissue cytokine mRNA production was assessed by real-time reverse transcription-polymerase chain reaction, and tissue and supernatant protein were evaluated by immunofluorescence, enzyme-linked immunosorbent assay, and Western blot. Results: Photobiomodulation with 660-nm wavelength light induced transcription of IL-1β and IL-6 mRNA and decreased that of IL-8. Tissue protein content of IL-6 and IL-8 was unchanged, whereas supernatant protein content of IL-8 was significantly increased (P=.023) by 1.5mW/cm2 treatment. To describe the localization of cytokines between tissue and supernatant, the relative diffusion of each was calculated and found to be 15-fold higher for IL-6 than for IL-8 despite an overall higher concentration of IL-8 in the tissue. Conclusion: In this study, photobiomodulation elicited mRNA and protein changes quantifiable in both the tissue and supernatant. In addition, the use of this advanced culture model allowed for histological assessment and the comparison of “local†versus “circulatory†responses between the tissue and supernatant, respectively. [ABSTRACT FROM AUTHOR]
- Published
- 2019
35. Heat transfer analysis and resolution quantification of active dynamic thermography through human skin.
- Author
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Prindeze, Nicholas J., Mann, Yvette V. L., Feric, Tony G., Currie, Timothy R., Carney, Bonnie C., Moffatt, Lauren T., Loew, Murray H., and Shupp, Jeffrey W.
- Published
- 2018
- Full Text
- View/download PDF
36. Matrix Metalloproteinases Are Differentially Regulated and Responsive to Compression Therapy in a Red Duroc Model of Hypertrophic Scar.
- Author
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Travis, Taryn E., Ghassemi, Pejhman, Prindeze, Nicholas J., Moffatt, Lauren T., Carney, Bonnie C., Alkhalil, Abdulnaser, Ramella-Roman, Jessica C., and Shupp, Jeffrey W.
- Subjects
MATRIX metalloproteinases ,HYPERTROPHIC scars ,COMPRESSION therapy ,EXTRACELLULAR matrix proteins ,WOUND healing - Abstract
Proteins of the matrix metalloproteinases family play a vital role in extracellular matrix maintenance and basic physiological processes in tissue homeostasis. The function and activities of matrix metalloproteinases in response to compression therapies have yet to be defined. Here, a swine model of hypertrophic scar was used to profile the transcription of all known 26 matrix metalloproteinases in scars treated with a precise compression dose. Methods: Full-thickness excisional wounds were created. Wounds underwent healing and scar formation. A subset of scars underwent 2 weeks of compression therapy. Biopsy specimens were preserved, and microarrays, reverse transcription-polymerase chain reaction, Western blotting, and immunohistochemistry were performed to characterize the transcription and expression of various matrix metalloproteinase family members. Results: Microarray results showed that 13 of the known 26 matrix metalloproteinases were differentially transcribed in wounds relative to the preinjury skin. The predominant upregulation of these matrix metalloproteinases during early wound-healing stages declined gradually in later stages of wound healing. The use of compression therapy reduced this decline in 10 of the 13 differentially regulated matrix metalloproteinases. Further investigation of MMP7 using reverse transcription-polymerase chain reaction confirmed the effect of compression on transcript levels. Assessment of MMP7 at the protein level using Western blotting and immunohistochemistry was concordant. Conclusions: In a swine model of hypertrophic scar, the application of compression to hypertrophic scar attenuated a trend of decreasing levels of matrix metalloproteinases during the process of hypertrophic wound healing, including MMP7, whose enzyme regulation was confirmed at the protein level. [ABSTRACT FROM AUTHOR]
- Published
- 2018
37. Reference ranges for rotational thromboelastometry in male Sprague Dawley rats.
- Author
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Vigiola Cruz, Mariana, Luker, Jenna N., Carney, Bonnie C., Brummel-Ziedins, Kathleen E., Bravo, Maria-Cristina, Orfeo, Thomas, Chen, Jason H., Moffatt, Lauren T., and Shupp, Jeffrey W.
- Subjects
ANIMAL experimentation ,BLOOD coagulation ,BLOOD coagulation disorders ,BLOOD coagulation tests ,RATS ,REFERENCE values ,THROMBELASTOGRAPHY ,LABORATORY equipment & supplies - Abstract
Background: A functional coagulation assay was used to investigate the extrinsic pathway of coagulation on citrated whole blood samples from healthy adult male Sprague Dawley rats using the mini cup and pin system. Methods: Reference values for coagulation parameters from forty-three animals were calculated using data obtained from the ROTEM® delta hemostasis analyzer with the EXTEM test. Results: The following ranges, presented as the 2.5-97.5 percentiles, were established: CT [18-77], CFT [20-80], α [73-86], MCF [53-70], and ML [1-22], along with others. Conclusions: These reference ranges can be used in future studies in rats to identify clinically significant coagulopathies. [ABSTRACT FROM AUTHOR]
- Published
- 2017
- Full Text
- View/download PDF
38. Disruption of Biofilms and Neutralization of Bacteria Using Hypochlorous Acid Solution: An In Vivo and In Vitro Evaluation.
- Author
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Day, Anna, Alkhalil, Abdulnaser, Carney, Bonnie C., Hoffman, Hilary N., Moffatt, Lauren T., and Shupp, Jeffrey W.
- Published
- 2017
- Full Text
- View/download PDF
39. Elastin Is Differentially Regulated by Pressure Therapy in a Porcine Model of Hypertrophic Scar.
- Author
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Carney, Bonnie C., Liu, Zekun, Alkhalil, Abdulnaser, Travis, Taryn E., Ramella-Roman, Jessica, Moffatt, Lauren T., and Shupp, Jeffrey W.
- Subjects
PROTEIN metabolism ,ANIMAL experimentation ,BIOLOGICAL models ,PENETRATING wounds ,PRESSURE ,STRETCH (Physiology) ,SWINE ,DISEASE complications ,HYPERTROPHIC scars ,THERAPEUTICS - Abstract
Beneficial effects of pressure therapy for hypertrophic scars have been reported, but the mechanisms of action are not fully understood. This study evaluated elastin and its contribution to scar pliability. The relationship between changes in Vancouver Scar Scale (VSS) scores of pressure-treated scars and differential regulation of elastin was assessed. Hypertrophic scars were created and assessed weekly using VSS and biopsy procurement. Pressure treatment began on day 70 postinjury. Treated scars were compared with untreated shams. Treatment lasted 2 weeks, through day 84, and scars were assessed weekly through day 126. Transcript and protein levels of elastin were quantified. Pressure treatment resulted in lower VSS scores compared with sham-treated scars. Pliability (VSSP) was a key contributor to this difference. At day 70 pretreatment, VSSP = 2. Without treatment, sham-treated scars became less pliable, while pressure-treated scars became more pliable. The percentage of elastin in scars at day 70 was higher than in uninjured skin. Following treatment, the percentage of elastin increased and continued to increase through day 126. Untreated sham scars did not show a similar increase. Quantification of Verhoeff-Van Gieson staining corroborated the findings and immunofluorescence revealed the alignment of elastin fibers. Pressure treatment results in increased protein level expression of elastin compared with sham-untreated scars. These findings further characterize the extracellular matrix's response to the application of pressure as a scar treatment, which will contribute to the refinement of rehabilitation practices and ultimately improvements in functional and psychosocial outcomes for patients. [ABSTRACT FROM AUTHOR]
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- 2017
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40. Effectiveness of a Glycylcycline Antibiotic for Reducing the Pathogenicity of Superantigen-Producing Methicillin-Resistant Staphylococcus aureus in Burn Wounds.
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Nosanov, Lauren B., Jo, Daniel Y., Randad, Pranay R., Moffatt, Lauren T., Carney, Bonnie C., Ortiz, Rachel T., and Shupp, Jeffrey W.
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BURN patients ,METHICILLIN resistance ,CLINDAMYCIN - Abstract
Objective: Burn-injured patients are highly susceptible to infectious complications, which are often associated with increased morbidity and mortality. Rates of antibiotic resistance have increased, and resistant species such as methicillin-resistant Staphylococcus aureus provide additional challenges in the form of virulence factors. Proteins can disrupt local healing, leading to systemic immune disruption. To optimize outcomes, treatments that reduce pathogenicity must be identified. This study aims to compare a glycylcycline antibiotic--tigecycline--with clindamycin for effectiveness in treating superantigenic methicillin-resistant Staphylococcus aureus in burn wounds. Methods: Sprague-Dawley rats received paired 2 × 2-cm burn wounds, which were subsequently inoculated with known virulence factor-producing methicillin-resistant Staphylococcus aureus or media alone on postinjury day 1. Infected animals received twice-daily tigecycline (high or low dose), twice-daily clindamycin (high or low dose), or saline alone (positive controls). Daily sampling and imaging assessments were performed. Results: Bacterial counts and toxin levels were reduced significantly in antibiotic-treated groups relative to positive controls (P < .001). Results from day 7 showed measurable toxin levels in clindamycin-treated, but not tigecycline-treated, wounds. Imaging analysis revealed a return of wound perfusion in tigecycline-treated animals similar to the sham animals. Transcript analysis using polymerase chain reaction and polymerase chain reaction arrays demonstrated downregulation of gene expression in antibiotic-treated animals as compared with positive controls. Conclusions: Overall, this study supports the use of tigecycline in the treatment of methicillin-resistant Staphylococcus aureus-infected burn wounds. While both protein synthesis inhibitors are effective, tigecycline appears to be superior in controlling toxin levels, enabling better wound healing. [ABSTRACT FROM AUTHOR]
- Published
- 2017
41. Active Dynamic Thermography is a Sensitive Method for Distinguishing Burn Wound Conversion.
- Author
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Prindeze, Nicholas J., Hoffman, Hilary A., Ardanuy, Jeremy G., Zhang, Jenny, Carney, Bonnie C., Moffatt, Lauren T., and Shupp, Jeffrey W.
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- 2016
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42. A new approach for optical assessment of directional anisotropy in turbid media.
- Author
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Ghassemi, Pejhman, Moffatt, Lauren T., Shupp, Jeffrey W., and Ramella‐Roman, Jessica C.
- Abstract
A study of polarized light transport in scattering media exhibiting directional anisotropy or linear birefringence is presented in this paper. Novel theoretical and experimental methodologies for the quantification of birefringent alignment based on out-of-plane polarized light transport are presented here. A polarized Monte Carlo model and a polarimetric imaging system were devised to predict and measure the impact of birefringence on an impinging linearly polarized light beam. Ex-vivo experiments conducted on bovine tendon, a biological sample consisting of highly packed type I collagen fibers with birefringent property, showed good agreement with the analytical results. [ABSTRACT FROM AUTHOR]
- Published
- 2016
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43. Examination of the Early Diagnostic Applicability of Active Dynamic Thermography for Burn Wound Depth Assessment and Concept Analysis.
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Prindeze, Nicholas J., Fathi, Payam, Mino, Matthew J., Mauskar, Neil A., Travis, Taryn E., Paul, Dereck W., Moffatt, Lauren T., and Shupp, Jeffrey W.
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- 2015
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44. Noninvasive imaging technologies for cutaneous wound assessment: A review.
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Paul, Dereck W., Ghassemi, Pejhman, Ramella‐Roman, Jessica C., Prindeze, Nicholas J., Moffatt, Lauren T., Alkhalil, Abdulnaser, and Shupp, Jeffrey W.
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INJURY complications ,TRAUMATOLOGY diagnosis ,WOUND & injury classification ,DIAGNOSTIC imaging ,MASS spectrometry ,MEDICAL thermography ,MICROSCOPY ,NEAR infrared spectroscopy ,PERFUSION ,RADIONUCLIDE imaging ,STATISTICS ,DATA analysis ,OPTICAL coherence tomography ,SEVERITY of illness index - Abstract
The ability to phenotype wounds for the purposes of assessing severity, healing potential and treatment is an important function of evidence-based medicine. A variety of optical technologies are currently in development for noninvasive wound assessment. To varying extents, these optical technologies have the potential to supplement traditional clinical wound evaluation and research, by providing detailed information regarding skin components imperceptible to visual inspection. These assessments are achieved through quantitative optical analysis of tissue characteristics including blood flow, collagen remodeling, hemoglobin content, inflammation, temperature, vascular structure, and water content. Technologies that have, to this date, been applied to wound assessment include: near infrared imaging, thermal imaging, optical coherence tomography, orthogonal polarization spectral imaging, fluorescence imaging, laser Doppler imaging, microscopy, spatial frequency domain imaging, photoacoustic detection, and spectral/hyperspectral imaging. We present a review of the technologies in use or development for these purposes with three aims: (1) providing basic explanations of imaging technology concepts, (2) reviewing the wound imaging literature, and (3) providing insight into areas for further application and exploration. Noninvasive imaging is a promising advancement in wound assessment and all technologies require further validation. [ABSTRACT FROM AUTHOR]
- Published
- 2015
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45. A portable automatic pressure delivery system for scar compression therapy in large animals.
- Author
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Ghassemi, Pejhman, Shupp, Jeffrey W., Travis, Taryn E., Gravunder, Andrew J., Moffatt, Lauren T., and Ramella-Roman, Jessica C.
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COMPRESSION therapy ,HYPERTROPHIC scars ,SCARS ,WOUNDS & injuries ,ANIMAL models in research ,PREVENTION - Abstract
Compression therapy has long been a standard treatment for hypertrophic scar prevention. However, due to the lack of objective, quantitative assessments, and measurements of scar severity, as well as the lack of a self-operated, controllable, and precise pressure delivery technique, limited concrete evidence exists, demonstrating compression therapy's efficacy. We have designed and built an automatic pressure delivery system to apply and maintain constant pressure on scar tissue in an animal model. A force sensor positioned on a compression plate reads the imposed force in real-time and sends the information to a feedback system controlling two position actuators. The actuators move accordingly to maintain a preset value of pressure onto the skin. The system was used in an in vivo model of compression therapy on hypertrophic scars. It was shown that the system was capable of delivering a constant pressure of 30 mmHg on scar wounds for a period of two weeks, and that phenotypic changes were seen in the wounds. [ABSTRACT FROM AUTHOR]
- Published
- 2015
- Full Text
- View/download PDF
46. Factors Impacting the Likelihood of Death in Patients with Small TBSA Burns.
- Author
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Travis, Taryn E., Moffatt, Lauren T., Jordan, Marion H., and Shupp, Jeffrey W.
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- 2015
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47. A Multimodal Assessment of Melanin and Melanocyte Activity in Abnormally Pigmented Hypertrophic Scar.
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Travis, Taryn E., Ghassemi, Pejhman, Ramella-Roman, Jessica C., Prindeze, Nicholas J., Paul, Dereck W., Moffatt, Lauren T., Jordan, Marion H., and Shupp, Jeffrey W.
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- 2015
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48. Regional neurovascular inflammation and apoptosis are detected after electrical contact injury.
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Prindeze, Nicholas J, Jo, Daniel Y, Paul, Dereck W, Ortiz, Rachel T, Carney, Bonnie C, Bullock, Rachel M, Moffatt, Lauren T, and Shupp, Jeffrey W
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- 2014
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49. 138 Evaluation of Healing Outcomes Combining Negative Pressure Wound Therapy with Autologous Skin Cell Suspension and Meshed Autografts: Pre-Clinical and Clinical Evidence.
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Carney, Bonnie C, Moffatt, Lauren T, Travis, Taryn E, Nisar, Saira, Keyloun, John W, Prindeze, Nicholas, Oliver, Mary, Kirkpatrick, Liam, Johnson, Laura S, and Shupp, Jeffrey W
- Subjects
NEGATIVE-pressure wound therapy ,CELL suspensions ,HEALING ,AUTOGRAFTS ,SKIN grafting - Abstract
Introduction Negative pressure wound therapy (NPWT) is an option for securing meshed split thickness skin grafts (mSTSGs) after burn excision to optimize skin graft adherence, working by minimizing disruption by shear forces and promoting the continual removal of wound bed drainage. Recently, the use of autologous skin cell suspension (ASCS) has been approved for use in treating full-thickness burn injuries in conjunction with mSTSGs. Limited data exists regarding the impact of NPWT on healing outcomes when the cellular suspension is utilized. It was hypothesized that NPWT in conjunction with ASCS+mSTSGs would aid in skin graft adherence without compromise to healing outcomes. Methods In this study, a Duroc pig model of burn, excision, mSTSG, ASCS + NPWT was used (n=2), where each animal had 2 sets of paired burns. Four wounds received mSTSG+ASCS+NPWT through post-operative day 3, and 4 wounds received mSTSG+ACSC+ traditional ASCS dressings. Percent re-epithelialization was measured using digital planimetry and Image J. Graft-adherence was evaluated using a scale with blinded reviewers (0=no graft loss, 4= >50% graft loss). Histological architecture, pigmentation, elasticity, and blood perfusion and blood vessel density were assessed at multiple time points through 2 weeks. After the evaluation of its effectiveness in animal models, the same surgical technique, including NPWT, was used in patients with full-thickness burns (n=9), and wound healing trajectories were described. Results In the Duroc pig study, all wounds healed within 14 days with minimal scar pathology and no significant differences in percent re-epithelialization between NPWT and non-NPWT wounds were observed (61.09 ± 9.01 and 61.15 ± 0.82% at Day 7). Additionally, no differences were detected for pigmentation, perfusion, or blood vessel density. Overall, the non-NPWT group had higher amounts of graft loss (1.0 ± 1.41 vs. 0 ± 0). NPWT-treated wounds had significantly improved elasticity (NPWT=109.5 ± 21.23 vs. non-NPWT=177.5 ± 35.4, p< 0.05). There were no differences in histological architecture between treatment groups. Patients had a median age of 53 (37–69), and median TBSA of 12.5 (8–18) resulting primarily from scald burns (67%). There were no reported morbidities, and all wounds were re-epithelialized within an expected time period. The use of NPWT promoted graft adherence, and was useful as a bolster dressing in wounds that crossed joints. Conclusions These data suggest the positive attributes of the cellular suspension delivered are retained following the application of NPWT. Re-epithelialization, revascularization, and repigmentation are not adversely impacted. [ABSTRACT FROM AUTHOR]
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- 2021
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50. 142 Transcriptome Analysis Captures Radiation Exposure in a Dose-sensitive Manner and Predicts Short-term Survival in a Mouse Model.
- Author
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Alkhalil, Abdulnaser, Clifford, John L, Miller, Stacy-Ann, Guatam, Aarti, Jett, Marti, Hammamieh, Rasha, Moffatt, Lauren T, and Shupp, Jeffrey W
- Subjects
RADIATION exposure ,SURVIVAL analysis (Biometry) ,EXPOSURE dose ,GENES ,SKIN biopsy ,RADIATION injuries - Abstract
Introduction A mass exposure to irradiation would be a challenge to health care systems. A simple tool or test that indicates the intensity of the absorbed radiation or the chances of survivability would be invaluable in this scenario. To identify biomarkers that potentially could provide novel biodosimetry tools, we have conducted a radiation dose-response and time-course experiment in mice that includes an assessment of the transcriptome of the skin. Methods Groups of mice (n=5) received whole-body X-ray exposures (0, 1, 3, 6, or 20Gy) and skin biopsies were obtained from each animal at times post-irradiation (h2, Days 4, 7, 21, 28). Biopsies were collected from the 20Gy cohort for only days 0, 4, and 7. Total RNA was isolated and microarrays were performed and analyzed using custom R scripts to obtain lists of probe sets differentially expressed. Changes in gene expression at Benjamini-Hochberg FDR adjusted P < 0.05 and FC >2 were deemed significant. Analyses were performed comparing the different doses of X-ray exposure over all time points. Results Mice in the 20Gy group were euthanized by d7 and the dose was considered lethal. Animals in 1, 3, and 6Gy groups completed the full experiment to d28. Sammon plot analysis of transcriptomes showed clear separation of samples based on the irradiation levels and time after exposure. The clearest separation was between samples of lethal and sublethal doses. Samples from animals exposed to sublethal doses separated more based on timepoints rather than the IR dose suggesting a level of similarity in the progression of the response to sublethal doses. Downregulation was the dominant modulation in the significantly differentially transcribed genes (SDTGs) in the 20Gy group. Temporal changes in ratios of upregulated/downregulated SDTGs (P < 0.05 and FC > 2) revealed further the difference between of transcriptome responses after exposure to lethal and sublethal doses and indicated a delayed peaks response with increasing IR doses within the sublethal range. About 59% of the SDTGs in 20gy were common to all timepoints while no more than 11% were common at the same duration in the other groups. Ratios of the number of SDTGs at h2 to those common to all TPs decreased in a dose-dependent manner with potential radiation dosimetric applications. Conclusions These results demonstrate a solid ability in detecting IR exposure, differentiating lethal and sublethal exposures, and differentiating among the exposure to sublethal doses. [ABSTRACT FROM AUTHOR]
- Published
- 2021
- Full Text
- View/download PDF
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