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301. In Vivo Persistence of Retrovirally Transduced Murine Long-Term Repopulating Cells Is Not Limited by Expression of Foreign Gene Products in the Fully or Minimally Myeloablated Setting

Author

Kang, Elizabeth, Giri, Neelam, Wu, Tong, Sellers, Stephanie, Kirby, Martha, Hanazono, Yutaka, Tisdale, John, and Dunbar, Cynthia E.

Abstract

Many nonmalignant hematologic disorders could potentially be treated by genetic correction of as few as 5-10% of target lineage cells. However, immune system clearance of cells expressing gene products perceived as foreign could be limiting. There is evidence that tolerance to foreign proteins can result when myeloablative conditioning is used, but this limits the overall applicability of such techniques. Therefore, we sought to evaluate the engraftment of hematopoietic stem cells carrying a foreign transgene after low-dose irradiation by comparing in vivo survival of murine long-term repopulating cells (LTRC) transduced with either a retroviral vector expressing the bacterial neomycin phosphotransferase gene (neo) or a vector containing neo gene sequences but modified to prevent protein expression (nonexpression). First, marrow cells from congenic donors were transduced with either vector and transplanted into recipients treated with standard dose irradiation of 800 rads. High-level engraftment and gene marking resulted, without differences in the marking levels or pattern of persistence of the cells between cells transduced with either vector. Low-dose irradiation at 100 rads was tested using higher cell doses. Marking levels as high as 10% overall were obtained, again with no differences between mice receiving cells transduced with the neo versus the nonexpression vectors. To investigate a potentially more immunogenic protein, marrow cells were transduced with a vector containing the green fluorescent protein (GFP) gene, and their persistence was studied in recipient mice receiving 100 rads. Stable GFP expression in 5-10% of circulating cells was observed long term. We conclude that even with very low dose conditioning, engraftment by genetically modified LTRC cells at clinically significant levels can be achieved without evidence for clearance of cells known to be expressing immunogenic proteins.

Published
2001
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302. Prolonged High-Level Detection of Retrovirally Marked Hematopoietic Cells in Nonhuman Primates after Transduction of CD34+Progenitors Using Clinically Feasible Methods

Author

Wu, Tong, Joon Kim, Hyeoung, Sellers, Stephanie E., Meade, Kristin E., Agricola, Brian A., Metzger, Mark E., Kato, Ikunoshin, Donahue, Robert E., Dunbar, Cynthia E., and Tisdale, John F.

Abstract

Low-level retroviral transduction and engraftment of hematopoietic long-term repopulating cells in large animals and humans remain primary obstacles to the successful application of hematopoietic stem cell (HSC) gene transfer in humans. Recent studies have reported improved efficiency by including stromal cells (STR), or the fibronectin fragment CH-296 (FN), and various cytokines such as flt3 ligand (FLT) during ex vivo culture and transduction in nonhuman primates. In this work, we extend our studies using the rhesus competitive repopulation model to further explore optimal and clinically feasible peripheral blood (PB) progenitor cell transduction methods. First, we compared transduction in the presence of either preformed autologous STR or immobilized FN. Long-term clinically relevant gene marking levels in multiple hematopoietic lineages from both conditions were demonstrated in vivo by semiquantitative PCR, colony PCR, and genomic Southern blotting, suggesting that FN could replace STR in ex vivo transduction protocols. Second, we compared transduction on FN in the presence of IL-3, IL-6, stem cell factor (SCF), and FLT (our best cytokine combination in prior studies) with a combination of megakaryocyte growth and development factor (MGDF), SCF, and FLT. Gene marking levels were equivalent in these animals, with no significant effect on retroviral gene transfer efficiency assessed in vivo by the replacement of IL-3 and IL-6 with MGDF. Our results indicate that SCF/G-CSF-mobilized PB CD34+cells are transduced with equivalent efficiency in the presence of either STR or FN, with stable long-term marking of multiple lineages at levels of 10–15% and transient marking as high as 54%. These results represent an advance in the field of HSC gene transfer using methods easily applied in the clinical setting.Molecular Therapy (2000) 1, 285–293; doi: 10.1006/mthe.2000.0034

Published
2000
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303. Engraftment of MDR1and NeoR Gene-Transduced Hematopoietic Cells After Breast Cancer Chemotherapy

Author

Moscow, Jeffrey A., Huang, Hui, Carter, Charles, Hines, Kenneth, Zujewski, JoAnne, Cusack, Georgie, Chow, Cathy, Venzon, David, Sorrentino, Brian, Chiang, Yawen, Goldspiel, Barry, Leitman, Susan, Read, Elizabeth J., Abati, Andrea, Gottesman, Michael M., Pastan, Ira, Sellers, Stephanie, Dunbar, Cynthia, and Cowan, Kenneth H.

Abstract

To determine whether the multidrug resistance gene MDR1could act as a selectable marker in human subjects, we studied engraftment of peripheral blood progenitor cells (PBPCs) transduced with either MDR1or the bacterial NeoR gene in six breast cancer patients. This study differed from previous MDR1gene therapy studies in that patients received only PBPCs incubated in retroviral supernatants (no nonmanipulated PBPCs were infused), transduction of PBPCs was supported with autologous bone marrow stroma without additional cytokines, and a control gene (NeoR) was used for comparison with MDR1. Transduced PBPCs were infused after high-dose alkylating agent therapy and before chemotherapy with MDR-substrate drugs. We found that hematopoietic reconstitution can occur using only PBPCs incubated ex vivo, that theMDR1gene product may play a role in engraftment, and that chemotherapy may selectively expand MDR1gene-transduced hematopoietic cells relative to NeoR transduced cells in some patients.

Published
1999
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304. Hypertrophic cardiomyopathy masquerading as sarcoidosis: cases illustrating cardiac imaging overlap relative to pathology.

Author

Sellers, Stephanie L., Ellis, Jennifer, Lai, Althea, Salcudean, Hannah, Reid, Anna B., Blanke, Philipp, McManus, Bruce M., Leipsic, Jonathon A., and Seidman, Michael A.

Subjects
*HYPERTROPHIC cardiomyopathy, *CARDIAC imaging, *CARDIAC magnetic resonance imaging, *HEART failure patients, *PATHOLOGY, *SARCOIDOSIS
Abstract

• Cardiac magnetic resonance imaging (MRI) is used to evaluate heart failure patients. • Features of sarcoidosis and end-stage HCM can have overlap on MRI. • Radiologists may mistake late-stage HCM as sarcoidosis due to similar MRI features. • Assessment of cardiac specimens provides correlation to prior MRI findings. • A multidisciplinary approach using both imaging and pathology aides patient diagnosis. [ABSTRACT FROM AUTHOR]

Published
2020
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305. Father Coyote.

Author

Sellers, Stephanie

Subjects
SHORT story (Literary form)
Abstract

The article presents the short story "Father Coyote," by Stephanie Sellers.

Published
2001

306. Ultrasound assessment of the posterolateral elbow ulnohumeral gap in normal subjects with and without posterolateral drawer testing

Author

Robertson, Nicola, McNabney, Charis, Chavda, Anesh, Flores, Dyan, Murphy, Kevin, Berkowitz, Yaron J., Roberts, David, Holmes, Kenneth R., Cresswell, Mark, Goetz, Thomas J., Hupin-Debeurme, Mathilde, Sellers, Stephanie L., and Murphy, Darra T.

Abstract

Posterolateral rotator instability (PLRI) is the most common pattern of recurrent elbow instability, and current imaging to aid PLRI diagnosis is limited. Thus, we sought to define use of ultrasound (US) to determine normal lateral ulnohumeral joint measurements, with and without posterolateral drawer testing to provide an insight into how US may aid diagnosis.

Published
2021
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308. Additional file 4 of Increased plasma lipid levels exacerbate muscle pathology in the mdx mouse model of Duchenne muscular dystrophy

Author

Milad, Nadia, White, Zoe, Tehrani, Arash, Sellers, Stephanie, Rossi, Fabio, and Bernatchez, Pascal

Subjects
2. Zero hunger, 3. Good health
Abstract

Figure S3. Animal body weights, heart weights, heart-body weight ratios, and cardiac histology. Body weight from 3 to 7 months on chow (A) and Western diets (B). Heart weight (C) and heart to body weight ratios (D) for groups at 7 months on Western diet. Examples of Masson’s trichrome stained hearts at 7 months of age on Western diet, scale bars 1 mm (left) and 250 μm (right) (E). Chow: WT (n = 3), ApoE (n = 5), mdx (n = 6), and mdx-ApoE (n = 11). Western: WT (n = 9), ApoE (n = 9), mdx (n = 5–11), and mdx-ApoE (n = 5–11). Mean ± SEM. *P

309. Additional file 4 of Increased plasma lipid levels exacerbate muscle pathology in the mdx mouse model of Duchenne muscular dystrophy

Author

Milad, Nadia, White, Zoe, Tehrani, Arash, Sellers, Stephanie, Rossi, Fabio, and Bernatchez, Pascal

Subjects
2. Zero hunger, 3. Good health
Abstract

Figure S3. Animal body weights, heart weights, heart-body weight ratios, and cardiac histology. Body weight from 3 to 7 months on chow (A) and Western diets (B). Heart weight (C) and heart to body weight ratios (D) for groups at 7 months on Western diet. Examples of Masson’s trichrome stained hearts at 7 months of age on Western diet, scale bars 1 mm (left) and 250 μm (right) (E). Chow: WT (n = 3), ApoE (n = 5), mdx (n = 6), and mdx-ApoE (n = 11). Western: WT (n = 9), ApoE (n = 9), mdx (n = 5–11), and mdx-ApoE (n = 5–11). Mean ± SEM. *P

310. Increased plasma lipid levels exacerbate muscle pathology in the mdx mouse model of Duchenne muscular dystrophy

Author

Milad, Nadia, White, Zoe, Tehrani, Arash Y, Sellers, Stephanie, Rossi, Fabio M, and Bernatchez, Pascal

Subjects
musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, lipids (amino acids, peptides, and proteins), 3. Good health
Abstract

Background: Duchenne muscular dystrophy (DMD) is caused by loss of dystrophin expression and leads to severe ambulatory and cardiac function decline. However, the dystrophin-deficient mdx murine model of DMD only develops a very mild form of the disease. Our group and others have shown vascular abnormalities in animal models of MD, a likely consequence of the fact that blood vessels express the same dystrophin-associated glycoprotein complex (DGC) proteins as skeletal muscles. Methods: To test the blood vessel contribution to muscle damage in DMD, mdx 4cv mice were given elevated lipid levels via apolipoprotein E (ApoE) gene knockout combined with normal chow or lipid-rich Western diets. Ambulatory function and heart function (via echocardiogram) were assessed at 4 and 7 months of age. After sacrifice, muscle histology and aortic staining were used to assess muscle pathology and atherosclerosis development, respectively. Plasma levels of total cholesterol, high-density lipoprotein (HDL), triglycerides, and creatine kinase (CK) were also measured. Results: Although there was an increase in left ventricular heart volume in mdx-ApoE mice compared to that in mdx mice, parameters of heart function were not affected. Compared with wild-type and ApoE-null, only mdx-ApoE KO mice showed significant ambulatory dysfunction. Despite no significant difference in plasma CK, histological analyses revealed that elevated plasma lipids in chow- and Western diet-fed mdx-ApoE mice was associated with severe exacerbation of muscle pathology compared to mdx mice: significant increase in myofiber damage and fibrofatty replacement in the gastrocnemius and triceps brachii muscles, more reminiscent of human DMD pathology. Finally, although both ApoE and mdx-ApoE groups displayed increased plasma lipids, mdx-ApoE exhibited atherosclerotic plaque deposition equal to or less than that of ApoE mice. Conclusions: Since others have shown that lipid abnormalities correlate with DMD severity, our data suggest that plasma lipids could be primary contributors to human DMD severity and that the notoriously mild phenotype of mdx mice might be attributable in part to their endogenously low plasma lipid profiles. Hence, DMD patients may benefit from lipid-lowering and vascular-targeted therapies.

312. Optimization of Enzymatic and Chemical Decellularization of Native Porcine Heart Valves for the Generation of Decellularized Xenografts.

Author

Saeid Nia, Monireh, Floder, Lena Maria, Seiler, Jette Anika, Puehler, Thomas, Pommert, Nina Sophie, Berndt, Rouven, Meier, David, Sellers, Stephanie L., Sathananthan, Janarthanan, Zhang, Xiling, Hasler, Mario, Gorb, Stanislav N., Warnecke, Gregor, and Lutter, Georg

Subjects
*HEART valves, *XENOGRAFTS, *HEART valve diseases, *TRITON X-100, *IMMUNE response, *TISSUE engineering
Abstract

One of the most important medical interventions for individuals with heart valvular disease is heart valve replacement, which is not without substantial challenges, particularly for pediatric patients. Due to their biological properties and biocompatibility, natural tissue-originated scaffolds derived from human or animal sources are one type of scaffold that is widely used in tissue engineering. However, they are known for their high potential for immunogenicity. Being free of cells and genetic material, decellularized xenografts, consequently, have low immunogenicity and, thus, are expected to be tolerated by the recipient's immune system. The scaffold ultrastructure and ECM composition can be affected by cell removal agents. Therefore, applying an appropriate method that preserves intact the structure of the ECM plays a critical role in the final result. So far, there has not been an effective decellularization technique that preserves the integrity of the heart valve's ultrastructure while securing the least amount of genetic material left. This study demonstrates a new protocol with untraceable cells and residual DNA, thereby maximally reducing any chance of immunogenicity. The mechanical and biochemical properties of the ECM resemble those of native heart valves. Results from this study strongly indicate that different critical factors, such as ionic detergent omission, the substitution of Triton X-100 with Tergitol, and using a lower concentration of trypsin and a higher concentration of DNase and RNase, play a significant role in maintaining intact the ultrastructure and function of the ECM. [ABSTRACT FROM AUTHOR]

Published
2024
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313. Tricuspid Regurgitation and TAVR: Outcomes, Risk Factors and Biomarkers.

Author

Puehler, Thomas, Pommert, Nina Sophie, Freitag-Wolf, Sandra, Seoudy, Hatim, Ernst, Markus, Haneya, Assad, Sathananthan, Janarthanan, Sellers, Stephanie L., Meier, David, Schöttler, Jan, Müller, Oliver J., Salehi Ravesh, Mona, Saad, Mohammed, Frank, Derk, and Lutter, Georg

Subjects
*HEART valve prosthesis implantation, *BRAIN natriuretic factor, *TRICUSPID valve insufficiency, MORTALITY risk factors
Abstract

Background. The significance of concomitant tricuspid regurgitation (TR) in the context of transcatheter aortic valve replacement (TAVR) remains unclear. This study aimed to analyze the severity of TR before and after TAVR with regard to short- and long-term survival and to analyze the influencing factors. Methods. In our retrospective analysis, TR before and after TAVR was examined and patients were classified into groups accordingly. Special attention was paid to patients with post-interventional changes in TR. Mortality after TAVR was considered the primary endpoint of the analysis and major complications according to the Valve Academic Research Consortium 3 (VARC3) were compared. Moreover, biomarkers and risk factors for worsening or improvement of TR through TAVR were analyzed. Results. Among 775 patients who underwent TAVR in our center between January 2009 and December 2019, 686 patients (89%) featured low- and 89 patients (11%) high-grade TR. High-grade pre-TAVR TR was associated with worse short- (30-day), mid- (2-year) and long-term survival up to 8 years. Even though in nearly half of the patients with high-grade TR the regurgitation improved within seven days after TAVR (n = 42/89), this did not result in a survival benefit for this subgroup. On the other hand, a worsening of low-grade TR was seen in more than 10% of the patients (n = 73/686), which was also associated with a worse prognosis. Predictors of worsening of TR after TAVR were adipositas, impaired right ventricular function and the presence of mild TR. Age, atrial fibrillation, COPD, impaired renal function and elevated cardiac biomarkers were risk factors for mortality after TAVR independent from the grade of TR. Conclusions. Not only pre-interventional, but also post-TAVR high-grade TR is associated with a worse prognosis after TAVR. TAVR can change concomitant tricuspid regurgitation, but improvement does not have any impact on short- and long-term survival. Worsening of TR after TAVR is possible and impairs the prognosis. [ABSTRACT FROM AUTHOR]

Published
2024
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314. Abstract 15977: Increased Inflammatory Monocytes in South Asians at Risk for Coronary Atherosclerosis

Author

Ramanathan, Krishnan, Franco, Christopher, Sellers, Stephanie, Whalen, Beth, Selvakumar, Kapilan, Nazzari, Hamed, Kiamanesh, Omid, Rolston, Thomas, Carolyn, Taylor M, and Leipsic, Jonathon

Abstract

Introduction:Global prevalence of coronary atherosclerosis (CAD) varies with ethnicity. South Asians (SA) have higher rates of cardiovascular morbidity and mortality compared to Caucasians (CA). Inflammation is a central mechanism in atherogenesis and inflammatory monocyte number are an independent predictor of this.Hypothesis:We evaluated inflammatory monocyte heterogeneity in a prospectively recruited population of Caucasian and South Asian.Methods:A prospective, consecutively enrolled cohort of patients, ages 19-69, with at least intermediate INTERHEART risk score for CAD were recruited from an outpatient population. Clinical parameters were obtained through history and physical exam findings. Monocyte heterogeneity was analyzed in a fluorescence activated cell scanner using dual color fluorescence (CD14, CD16) within the monocyte gate by trained staff blinded to clinical information. Percentage gated cells were compared using Student?s t-test and clinical data by Chi square test.Results:The study cohort comprised of 60 CA and 58 SA patients. The CA group consisted of 36% female with a mean age of 58-y and the SA group was made up of 46% female with a mean age of 54-y. Similar rates of smoking, hypertension, hypercholesterolemia and family history of CAD were seen in SA and CA. The SA patients had increased frequency of a history of diabetes (33% SA vs. 16% CA, P<0.05). The mean HbA1c (%) and Apo B- 100 (g/L) levels were numerically similar in both SA and CA. The percentage of inflammatory monocytes (CD14+/16-) was higher in the SA group (69.9 +8.9 vs.65.7 +11 %; p<0.05) compared to the CA group. The percentage of intermediate monocytes (CD14+/CD16+/-) was lower in the SA group (13.1 +5.7 vs. 17.9 +9.2% ; p<0.05 compared to the CA group. No differences were observed in the percentage of non-inflammatory monocytes (CD14+/16+) between groups (12.8 +4.7 in SA vs. 11.7 +4.4 % in CA; P>0.05).Conclusions:The frequency of CD14+/CD16- inflammatory monocytes is increased in stable South Asian at risk for coronary atheroscleosis. Inflammation may be an important driver of increased cardiovascular risk in South Asians. Our findings support the need for further research to address the growing epidemic of atherosclerotic heart disease amongst all South Asians.

Published
2019
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315. Molecular Coronary Plaque Imaging Using 18F-Fluoride

Author

Moss, Alastair J., Doris, Mhairi K., Andrews, Jack P.M., Bing, Rong, Daghem, Marwa, van Beek, Edwin J. R., Forsyth, Laura, Shah, Anoop S.V., Williams, Michelle C., Sellers, Stephanie, Leipsic, Jonathon, Dweck, Marc R., Parker, Richard A., Newby, David E., and Adamson, Philip D.

Abstract

Supplemental Digital Content is available in the text.

Published
2019
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316. Producing and Testing Prototype Tissue-Engineered 3D Tri-Leaflet Valved Stents on Biodegradable Poly-ε-Caprolactone Scaffolds.

Author

Lutter, Georg, Pommert, Nina Sophie, Zhang, Xiling, Seiler, Jette, Saeid Nia, Monireh, Meier, David, Sellers, Stephanie L., Gorb, Stanislav N., Hansen, Jan-Hinnerk, Seoudy, Hatim, Müller, Oliver J., Saad, Mohammed, Haneya, Assad, Frank, Derk, Puehler, Thomas, and Sathananthan, Janarthanan

Subjects
*PROSTHETIC heart valves, *PULMONARY valve, *MECHANICAL hearts, *HEART valves, *NANOFIBERS, *SCANNING electron microscopy, *FLUORESCENCE microscopy
Abstract

Transcatheter pulmonary valve replacement is a minimally-invasive alternative treatment for right ventricular outflow tract dysfunction and has been rapidly evolving over the past years. Heart valve prostheses currently available still have major limitations. Therefore, one of the significant challenges for the future is the roll out of transcatheter tissue engineered pulmonary valve replacement to more patients. In the present study, biodegradable poly-ε-caprolactone (PCL) nanofiber scaffolds in the form of a 3D leaflet matrix were successfully seeded with human endothelial colony-forming cells (ECFCs), human induced pluripotent stem cell-derived MSCs (hMSCs), and porcine MSCs (pMSCs) for three weeks for the generation of 3D tissue-engineered tri-leaflet valved stent grafts. The cell adhesion, proliferation, and distribution of these 3D heart leaflets was analyzed using fluorescence microscopy and scanning electron microscopy (SEM). All cell lineages were able to increase the overgrown leaflet area within the three-week timeframe. While hMSCs showed a consistent growth rate over the course of three weeks, ECFSs showed almost no increase between days 7 and 14 until a growth spurt appeared between days 14 and 21. More than 90% of heart valve leaflets were covered with cells after the full three-week culturing cycle in nearly all leaflet areas, regardless of which cell type was used. This study shows that seeded biodegradable PCL nanofiber scaffolds incorporated in nitinol or biodegradable stents will offer a new therapeutic option in the future. [ABSTRACT FROM AUTHOR]

Published
2023
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318. Detection and Prediction of Bioprosthetic Aortic Valve Degeneration.

Author

Cartlidge, Timothy R.G., Doris, Mhairi K., Sellers, Stephanie L., Pawade, Tania A., White, Audrey C., Pessotto, Renzo, Kwiecinski, Jacek, Fletcher, Alison, Alcaide, Carlos, Lucatelli, Christophe, Densem, Cameron, Rudd, James H.F., van Beek, Edwin J.R., Tavares, Adriana, Virmani, Renu, Berman, Daniel, Leipsic, Jonathon A., Newby, David E., and Dweck, Marc R.

Subjects
*AORTIC valve
Abstract

Background: Bioprosthetic aortic valve degeneration is increasingly common, often unheralded, and can have catastrophic consequences.Objectives: The authors sought to assess whether 18F-fluoride positron emission tomography (PET)-computed tomography (CT) can detect bioprosthetic aortic valve degeneration and predict valve dysfunction.Methods: Explanted degenerate bioprosthetic valves were examined ex vivo. Patients with bioprosthetic aortic valves were recruited into 2 cohorts with and without prosthetic valve dysfunction and underwent in vivo contrast-enhanced CT angiography, 18F-fluoride PET, and serial echocardiography during 2 years of follow-up.Results: All ex vivo, degenerate bioprosthetic valves displayed 18F-fluoride PET uptake that colocalized with tissue degeneration on histology. In 71 patients without known bioprosthesis dysfunction, 14 had abnormal leaflet pathology on CT, and 24 demonstrated 18F-fluoride PET uptake (target-to-background ratio 1.55 [interquartile range (IQR): 1.44 to 1.88]). Patients with increased 18F-fluoride uptake exhibited more rapid deterioration in valve function compared with those without (annualized change in peak transvalvular velocity 0.30 [IQR: 0.13 to 0.61] vs. 0.01 [IQR: -0.05 to 0.16] ms-1/year; p < 0.001). Indeed 18F-fluoride uptake correlated with deterioration in all the conventional echocardiographic measures of valve function assessed (e.g., change in peak velocity, r = 0.72; p < 0.001). Each of the 10 patients who developed new overt bioprosthesis dysfunction during follow-up had evidence of 18F-fluoride uptake at baseline (target-to-background ratio 1.89 [IQR: 1.46 to 2.59]). On multivariable analysis, 18F-fluoride uptake was the only independent predictor of future bioprosthetic dysfunction.Conclusions: 18F-fluoride PET-CT identifies subclinical bioprosthetic valve degeneration, providing powerful prediction of subsequent valvular dysfunction and highlighting patients at risk of valve failure. This technique holds major promise in the diagnosis of valvular degeneration and the surveillance of patients with bioprosthetic valves. (18F-Fluoride Assessment of Aortic Bioprosthesis Durability and Outcome [18F-FAABULOUS]; NCT02304276). [ABSTRACT FROM AUTHOR]

Published
2019
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319. Long-Distance Gifts: For Paula Gunn Allen.

Author

Sellers, Stephanie A.

Subjects
LONG-Distance Gifts: For Paula Gunn Allen (Poem), SELLERS, Stephanie A.
Abstract

The article presents the poem "Long-Distance Gifts: For Paula Gunn Allen," by Stephanie A. Sellers. First line: Look into the palms of these hands; Last line: I tell jokes, then sit on the porch with my drum and sing.

Published
2008

320. Shaking the Pumpkin.

Author

Sellers, Stephanie

Subjects
SHAKING the Pumpkin (Poem), SELLERS, Stephanie
Abstract

The poem "Shaking the Pumpkin," by Stephanie Sellers is presented. First Line: all my life, shaking this; Last Line: awakens on my tongue.

Published
2014

322. The Effect of Evidence Quality, Source Expertise, and Personal Involvement on Attitude Change: A Conceptual Replication of Petty, Cacioppo, and Goldman (1981).

Author

Chung, Sungeun, McLaughlin, Meghan, Wentzel, Ashely, Churchill, Hilary, Flores, Gordillo, Galvan, Natalia, MARICLE, MEAGAN, Marlette, Janet, Pingolt, Steven, Sellers, Stephanie, Strattman, Jessica, and Tedla, Hanna

Subjects
QUALITY, EXPERTISE, ENGAGEMENT (Philosophy), TRUTHFULNESS & falsehood, ATTITUDE (Psychology)
Abstract

Two models about the effect of evidence quality, source expertise, and personal involvement on post-message attitudes were tested with a conceptual replication of Petty, Cacioppo, and Goldman's (1981) experiment (N = 386). Evidence quality had a positive effect on both perceived argument quality and perceived source credibility. Source expertise had a positive effect on perceived source credibility. Personal involvement had a negative effect on both perceived argument quality and perceived source credibility. Perceived argument quality had a positive effect on post-message attitudes. The effect of evidence quality and source expertise on attitudes did not differ between high and low personal involvement. The discrepancies in results between the original and the replicated studies were discussed. ..PAT.-Unpublished Manuscript [ABSTRACT FROM AUTHOR]

Published
2010

323. Transcatheter Aortic Valve Implantation by Intercostal Access: Initial Experience with a No-Touch Technique.

Author

Pommert, Nina Sophie, Zhang, Xiling, Puehler, Thomas, Seoudy, Hatim, Huenges, Katharina, Schoettler, Jan, Haneya, Assad, Friedrich, Christine, Sathananthan, Janarthanan, Sellers, Stephanie L., Meier, David, Mueller, Oliver J., Saad, Mohammed, Frank, Derk, and Lutter, Georg

Subjects
*HEART valve prosthesis implantation, *THORACOTOMY, *CORONARY artery bypass, *AORTIC stenosis, *AORTIC valve diseases, *PERIPHERAL vascular diseases, *PERCUTANEOUS coronary intervention
Abstract

Background: Transcatheter aortic valve implantation (TAVI) is now a well-established therapeutic option in an elderly high-risk patient cohort with aortic valve disease. Although most commonly performed via a transfemoral route, alternative approaches for TAVI are constantly being improved. Instead of the classical mini-sternotomy, it is possible to achieve a transaortic access via a right anterior mini-thoracotomy in the second intercostal space. We describe our experience with this sternum- and rib-sparing technique in comparison to the classical transaortic approach. Methods: Our retrospective study includes 173 patients who were treated in our institution between January 2017 and April 2020 with transaortic TAVI via either upper mini-sternotomy or intercostal thoracotomy. The primary endpoint was 30-day mortality, and secondary endpoints were defined as major postoperative complications that included admission to the intensive care unit and overall hospital stay, according to the Valve Academic Research Consortium 3. Results: Eighty-two patients were treated with TAo-TAVI by upper mini-sternotomy, while 91 patients received the intercostal approach. Both groups were comparable in age (mean age: 82 years) and in the proportion of female patients. The intercostal group had a higher rate of peripheral artery disease (41% vs. 22%, p = 0.008) and coronary artery disease (71% vs. 40%, p < 0.001) with a history of percutaneous coronary intervention or coronary artery bypass grafting, resulting in significantly higher preinterventional risk evaluation (EuroScore II 8% in the intercostal vs. 4% in the TAo group, p = 0.005). Successful device implantation and a reduction of the transvalvular gradient were achieved in all cases with a significantly lower rate of trace to mild paravalvular leakage in the intercostal group (12% vs. 33%, p < 0.001). The intercostal group required significantly fewer blood transfusions (0 vs. 2 units, p = 0.001) and tended to require less reoperation (7% vs. 15%, p = 0.084). Hospital stays (9 vs. 12 d, p = 0.011) were also shorter in the intercostal group. Short- and long-term survival in the follow-up showed comparable results between the two approaches (30-day, 6-month- and 2-year mortality: 7%, 23% and 36% in the intercostal vs. 9%, 26% and 33% in the TAo group) with acute kidney injury (AKI) and reintubation being independent risk factors for mortality. Conclusions: Transaortic TAVI via an intercostal access offers a safe and effective treatment of aortic valve stenosis. [ABSTRACT FROM AUTHOR]

Published
2023
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324. TCT-968 Automatic Echocardiography Prompts Reveal Lack of Equitable Access to Care in Patients With Tricuspid Regurgitation: The Equitable Access Study III.

Author

Offen, Sophie, Johns, Sarah, Boone, Terra, Kersche, Georgia, Robinson, Brady, Wang, Jia, Kulyk, Katherine, Jelisejevas, Julius, Husain, Ali, Millar, Kevin, Ogran, Hassan, Tsang, Teresa, Luong, Christina, Yeung, Darwin, Tsang, Michael, Tang, Erin, Sellers, Stephanie, Moss, Robert, Thompson, Christopher, and Sathananthan, Gnalini

Subjects
*TRICUSPID valve insufficiency, *ECHOCARDIOGRAPHY, *PATIENT care
Published
2024
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326. TCT-830 Feasibility and Utility of Anatomic and Physiological Evaluation of Coronary Disease With Cardiac CT in Severe Aortic Stenosis (FUTURE-AS Registry).

Author

Ihdayhid, Abdul Rahman, Polsani, Venkateshwar, Fairbairn, Timothy, Fitzgibbons, Timothy, Ko, Brian, Liu, Shizhen, Khoo, John, Coughlan, Fionn, Shetty, Sharad, Chatfield, Andrew, Akodad, Mariama, Raju, Vikram, Kakouros, Nikolaos, Lewin, Stephen, Sathananthan, Janarthanan, Webb, John, Wood, David, Leipsic, Jonathon, and Sellers, Stephanie

Subjects
*CORONARY disease, *AORTIC stenosis
Published
2024
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327. TCT-652 Feasibility and Utility of Anatomical and Physiological Evaluation of Coronary Disease With Cardiac CT in Severe Aortic Stenosis (FUTURE-AS Registry).

Author

Ihdayhid, Abdul Rahman, Polsani, Venkateshwar, Fairbairn, Timothy, Fitzgibbons, Timothy, Ko, Brian, Liu, Shizhen, Khoo, John, Coughlan, Fionn, Shetty, Sharad, Chatfield, Andrew, Akodad, Mariama, Raju, Vikram, Kakouros, Nikolaos, Lewin, Stephen, Sathananthan, Janarthanan, Webb, John, Wood, David, Leipsic, Jonathon, and Sellers, Stephanie

Subjects
*CORONARY disease, *AORTIC stenosis
Published
2024
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328. TCT-611 Automatic Echocardiography Prompts Reveal Lack of Equitable Access to Care in Patients With Mitral Regurgitation: The Equitable Access Study II.

Author

Offen, Sophie, Johns, Sarah, Boone, Terra, Kersche, Georgia, Kulyk, Katherine, Robinson, Brady, Wang, Jia, Jelisejevas, Julius, Husain, Ali, Millar, Kevin, Ogran, Hassan, Tsang, Teresa, Luong, Christina, Yeung, Darwin, Tsang, Michael, Moss, Robert, Sathananthan, Gnalini, Thompson, Christopher, Tang, Erin, and Sellers, Stephanie

Subjects
*MITRAL valve insufficiency, *ECHOCARDIOGRAPHY, *PATIENT care
Published
2024
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330. Looking Good.

Author

Sellers, Stephanie A.

Abstract

A letter to the editor is presented which is concerned with images of women which are contained in issues of the periodical "Yoga Journal."

Published
2011

332. Late Balloon Valvuloplasty for Transcatheter Heart Valve Dysfunction.

Author

Akodad, Mariama, Blanke, Philipp, Chuang, Ming-Yu A., Duchscherer, Jade, Sellers, Stephanie L., Chatfield, Andrew G., Gulsin, Gaurav G., Lauck, Sandra, Leipsic, Jonathon A., Meier, David, Moss, Rob R., Cheung, Anson, Sathananthan, Janarthanan, Wood, David A., Ye, Jian, and Webb, John G.

Subjects
*PERCUTANEOUS balloon valvuloplasty, *HEART valves, *HEART valve prosthesis implantation, *AORTIC stenosis, *TREATMENT effectiveness, *PROSTHETIC heart valves, *CATHETERIZATION, *PROSTHESIS design & construction, AORTIC valve surgery
Abstract

Background: Transcatheter heart valve (THV) dysfunction with an elevated gradient or paravalvular leak (PVL) may be documented late after THV implantation. Medical management, paravalvular plugs, redo THV replacement, or surgical valve replacement may be considered. However, late balloon dilatation is rarely utilized because of concerns about safety or lack of efficacy.Objectives: We aimed to evaluate the safety and efficacy of late dilatation in the management of THV dysfunction.Methods: All patients who underwent late dilatation for symptomatic THV dysfunction at 2 institutions between 2016 and 2021 were identified. Baseline, procedural characteristics, and clinical and echocardiographic outcomes were documented. THV frame expansion was assessed by multislice computed tomography before and after late dilatation.Results: Late dilatation was performed in 30 patients a median of 4.6 months (IQR: 2.3-11.0 months) after THV implantation in the aortic (n = 25; 83.3%), mitral (n = 2; 6.7%), tricuspid (n = 2; 6.7%) and pulmonary (n = 1; 3.3%) position. THV underexpansion was documented at baseline, and frame expansion substantially improved after late dilatation. The mean transvalvular gradient fell in all patients. For aortic THVs specifically, mean transaortic gradient fell from 25.4 ± 13.9 mm Hg to 10.8 ± 4.1 mm Hg; P < 0.001. PVL was reduced to ≤mild in all 11 patients with a previous >mild PVL. Embolic events, stroke, annular injury, and bioprosthetic leaflet injury were not observed. Symptomatic benefit was durable at 19.6 months (IQR: 14.8-36.1 months) follow-up.Conclusions: Balloon dilatation late after THV implantation appears feasible and safe in appropriately selected patients and may result in THV frame expansion resulting in improvements in hemodynamic performance and PVL. [ABSTRACT FROM AUTHOR]

Published
2022
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333. Personalized intervention cardiology with transcatheter aortic valve replacement made possible with a non-invasive monitoring and diagnostic framework.

Author

Khodaei, Seyedvahid, Henstock, Alison, Sadeghi, Reza, Sellers, Stephanie, Blanke, Philipp, Leipsic, Jonathon, Emadi, Ali, and Keshavarz-Motamed, Zahra

Subjects
*HEART valve prosthesis implantation, *AORTIC stenosis, *CARDIOVASCULAR diseases, *BLOOD flow, *HEART function tests
Abstract

One of the most common acute and chronic cardiovascular disease conditions is aortic stenosis, a disease in which the aortic valve is damaged and can no longer function properly. Moreover, aortic stenosis commonly exists in combination with other conditions causing so many patients suffer from the most general and fundamentally challenging condition: complex valvular, ventricular and vascular disease (C3VD). Transcatheter aortic valve replacement (TAVR) is a new less invasive intervention and is a growing alternative for patients with aortic stenosis. Although blood flow quantification is critical for accurate and early diagnosis of C3VD in both pre and post-TAVR, proper diagnostic methods are still lacking because the fluid-dynamics methods that can be used as engines of new diagnostic tools are not well developed yet. Despite remarkable advances in medical imaging, imaging on its own is not enough to quantify the blood flow effectively. Moreover, understanding of C3VD in both pre and post-TAVR and its progression has been hindered by the absence of a proper non-invasive tool for the assessment of the cardiovascular function. To enable the development of new non-invasive diagnostic methods, we developed an innovative image-based patient-specific computational fluid dynamics framework for patients with C3VD who undergo TAVR to quantify metrics of: (1) global circulatory function; (2) global cardiac function as well as (3) local cardiac fluid dynamics. This framework is based on an innovative non-invasive Doppler-based patient-specific lumped-parameter algorithm and a 3-D strongly-coupled fluid-solid interaction. We validated the framework against clinical cardiac catheterization and Doppler echocardiographic measurements and demonstrated its diagnostic utility by providing novel analyses and interpretations of clinical data in eleven C3VD patients in pre and post-TAVR status. Our findings position this framework as a promising new non-invasive diagnostic tool that can provide blood flow metrics while posing no risk to the patient. The diagnostic information, that the framework can provide, is vitally needed to improve clinical outcomes, to assess patient risk and to plan treatment. [ABSTRACT FROM AUTHOR]

Published
2021
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335. Ex vivo 18F-fluoride uptake and hydroxyapatite deposition in human coronary atherosclerosis.

Author

Moss, Alastair J., Sim, Alisia M., Adamson, Philip D., Seidman, Michael A., Andrews, Jack P. M., Doris, Mhairi K., Shah, Anoop S. V., BouHaidar, Ralph, Alcaide-Corral, Carlos J., Williams, Michelle C., Leipsic, Jonathon A., Dweck, Marc R., MacRae, Vicky E., Newby, David E., Tavares, Adriana A. S., and Sellers, Stephanie L.

Subjects
*ACUTE coronary syndrome, *CALCIFICATIONS of the breast, *RADIOACTIVE tracers, *HYDROXYAPATITE, *OSTEOPONTIN
Abstract

Early microcalcification is a feature of coronary plaques with an increased propensity to rupture and to cause acute coronary syndromes. In this ex vivo imaging study of coronary artery specimens, the non-invasive imaging radiotracer, 18F-fluoride, was highly selective for hydroxyapatite deposition in atherosclerotic coronary plaque. Specifically, coronary 18F-fluoride uptake had a high signal to noise ratio compared with surrounding myocardium that makes it feasible to identify coronary mineralisation activity. Areas of 18F-fluoride uptake are associated with osteopontin, an inflammation-associated glycophosphoprotein that mediates tissue mineralisation, and Runt-related transcription factor 2, a nuclear protein involved in osteoblastic differentiation. These results suggest that 18F-fluoride is a non-invasive imaging biomarker of active coronary atherosclerotic mineralisation. [ABSTRACT FROM AUTHOR]

Published
2020
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337. Effects of renin-angiotensin-aldosterone-system inhibitors on coronary atherosclerotic plaques: The PARADIGM registry.

Author

Williams, Curtis, Han, Donghee, Takagi, Hidenobu, Fordyce, Christopher B., Sellers, Stephanie, Blanke, Philipp, Lin, Fay Y., Shaw, Leslee J., Lee, Sang-Eun, Andreini, Daniele, Al-Mallah, Mouaz H., Budoff, Matthew J., Cademartiri, Filippo, Chinnaiyan, Kavitha, Choi, Jung Hyun, Conte, Edoardo, Marques, Hugo, de Araújo Gonçalves, Pedro, Gottlieb, Ilan, and Hadamitzky, Martin

Subjects
*ATHEROSCLEROTIC plaque, *ANGIOTENSIN-receptor blockers, *CORONARY angiography, *ACE inhibitors, *CORONARY artery disease, *BETA (Finance), *MEDICAL registries
Abstract

Inhibition of Renin-Angiotensin-Aldosterone-System (RAAS) has been hypothesized to improve endothelial function and reduce plaque inflammation, however, their impact on the progression of coronary atherosclerosis is unclear. We aim to study the effects of RAAS inhibitor on plaque progression and composition assessed by serial coronary CT angiography (CCTA). We performed a prospective, multinational study consisting of a registry of patients without history of CAD, who underwent serial CCTAs. Patients using RAAS inhibitors were propensity matched to RAAS inhibitor naïve patients based on clinical and CCTA characteristics at baseline. Atherosclerotic plaques in CCTAs were quantitatively analyzed for percent atheroma volume (PAV) according to plaque composition. Interactions between RAAS inhibitor use and baseline PAV on plaque progression were assessed in the unmatched cohort using a multivariate linear regression model. Of 1248 patients from the registry, 299 RAAS inhibitor taking patients were matched to 299 RAAS inhibitor naïve patients. Over a mean interval of 3.9 years, there was no significant difference in annual progression of total PAV between RAAS inhibitor naïve vs taking patients (0.75 vs 0.79%/year, p = 0.66). With interaction testing in the unmatched cohort, however, RAAS inhibitor use was significantly associated with lower non-calcified plaque progression (Beta coefficient −0.100, adjusted p = 0.038) with higher levels of baseline PAV. The use of RAAS inhibitors over a period of nearly 4 years did not significantly impact on total atherosclerotic plaque progression or various plaque components. However, interaction testing to assess the differential effect of RAAS inhibition based on baseline PAV suggested a significant decrease in progression of non-calcified plaque in patients with a higher burden of baseline atherosclerosis, which should be considered hypothesis generating. [Display omitted] • The effect of ACE inhibitors and ARBs on coronary plaque progression is unclear. • Serial coronary CT angiograms allows plaque burden to be assessed over time. • Using propensity matching, plaque progression stratified by ACE/ARB use was performed. • Overall, ACE/ARB use had no significant effect on plaque progression or morphology. [ABSTRACT FROM AUTHOR]

Published
2023
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338. TCT-519 Timing of Bioprosthetic Valve Fracture in Transcatheter Valve-in-Valve Intervention: Impact on Valve Durability and Leaflet Integrity.

Author

Meier, David, Payne, Geoffrey, Mostaço-Guidolin, Leila, Bouchareb, Rihab, Rich, Courtney, Lai, Althea, Chatfield, Andrew, Akodad, Mariama, Salcudean, Hannah, Puehler, Thomas, Pibarot, Philippe, Allen, Keith, Chhatriwalla, Adnan, Sondergaard, Lars, Wood, David, Webb, John, Leipsic, Jonathon, Sathananthan, Janarthanan, and Sellers, Stephanie

Subjects
*BIOPROSTHETIC heart valves, *DURABILITY, *PAMPHLETS
Published
2022
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343. Recombinant Decorin Fusion Protein Attenuates Murine Abdominal Aortic Aneurysm Formation and Rupture

Author

Tero A. H. Järvinen, Hongyan Zhao, Valerio Russo, Tatjana Bozin, Matthew R. Zeglinski, Bruce M. McManus, Yulia Merkulova, R. Chris Bleackley, Zhengguo Wu, Haishan Zeng, Michael A. Seidman, Stephanie Santacruz, Lubos Bohunek, David J. Granville, Yue Shen, Erkki Ruoslahti, Stephanie L. Sellers, Keerit Tauh, Cameron Oram, Christopher T. Turner, Lääketieteen ja biotieteiden tiedekunta - Faculty of Medicine and Life Sciences, University of Tampere, Shen, Yue, Russo, Valerio, Zeglinski, Matthew R, Sellers, Stephanie L, Wu, Zhengguo, Oram, Cameron, Santacruz, Stephanie, Merkulova, Yulia, Turner, Christopher, Tauh, Keerit, Zhao, Hongyan, Bozin, Tatjana, Bohunek, Lubos, Zeng, Haishan, Seidman, Michael A, Bleackley, R Chris, McManus, Bruce M, Ruoslahti, Erkki, Jarvinen, Tero AH, and Granville, David J

Subjects
0301 basic medicine, Apolipoprotein E, Pathology, medicine.medical_specialty, pulmonary, Decorin, lcsh:Medicine, Article, Mice, 03 medical and health sciences, Aortic aneurysm, Apolipoproteins E, medicine, otorhinolaryngologic diseases, Animals, Humans, recombinant, lcsh:Science, Mice, Knockout, decorin, DCN, Multidisciplinary, 030102 biochemistry & molecular biology, biology, Biolääketieteet – Biomedicine, business.industry, Angiotensin II, lcsh:R, Fibrillogenesis, medicine.disease, Fusion protein, Recombinant Proteins, Abdominal aortic aneurysm, Disease Models, Animal, 030104 developmental biology, Proteoglycan, biology.protein, cardiovascular system, lcsh:Q, business, Aortic Aneurysm, Abdominal, Farmasia - Pharmacy
Abstract

Decorin (DCN) is a small-leucine rich proteoglycan that mediates collagen fibrillogenesis, organization, and tensile strength. Adventitial DCN is reduced in abdominal aortic aneurysm (AAA) resulting in vessel wall instability thereby predisposing the vessel to rupture. Recombinant DCN fusion protein CAR-DCN was engineered with an extended C-terminus comprised of CAR homing peptide that recognizes inflamed blood vessels and penetrates deep into the vessel wall. In the present study, the role of systemically-administered CAR-DCN in AAA progression and rupture was assessed in a murine model. Apolipoprotein E knockout (ApoE-KO) mice were infused with angiotensin II (AngII) for 28 days to induce AAA formation. CAR-DCN or vehicle was administrated systemically until day 15. Mortality due to AAA rupture was significantly reduced in CAR-DCN-treated mice compared to controls. Although the prevalence of AAA was similar between vehicle and CAR-DCN groups, the severity of AAA in the CAR-DCN group was significantly reduced. Histological analysis revealed that CAR-DCN treatment significantly increased DCN and collagen levels within the aortic wall as compared to vehicle controls. Taken together, these results suggest that CAR-DCN treatment attenuates the formation and rupture of Ang II-induced AAA in mice by reinforcing the aortic wall.

Published
2017

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