37 results on '"Payne, Geoffrey W."'
Search Results
2. Impact of sex on microvascular reactivity in a murine model of diet-induced obesity and insulin resistance
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Sidsworth, Danielle A., Sellers, Stephanie L., Reutens-Hernandez, Jennifer P., Dunn, Elizabeth A., Gray, Sarah L., and Payne, Geoffrey W.
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- 2021
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3. Impact of Over-Expansion on SAPIEN 3 Transcatheter Heart Valve Pericardial Leaflets
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Sellers, Stephanie L., Sathananthan, Janarthanan, Bouchareb, Rihab, Mostaço-Guidolin, Leila B., Lau, Karen PL, Bugis, Joshua, Hensey, Mark, Blanke, Philipp, Payne, Geoffrey W., Lebeche, Djamel, Pibarot, Phillippe, Hackett, Tillie-Louise, Webb, John G., and Leipsic, Jonathon A.
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- 2020
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4. Impact of sublingual nitroglycerin dosage on FFRCT assessment and coronary luminal volume–to–myocardial mass ratio
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Holmes, Kenneth R., Fonte, Tim A., Weir-McCall, Jonathan, Anastasius, Malcolm, Blanke, Philipp, Payne, Geoffrey W., Ellis, Jen, Murphy, Darra T., Taylor, Charles, Leipsic, Jonathon A., and Sellers, Stephanie L.
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- 2019
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5. Hypertrophic Cardiomyopathy (HCM): New insights into Coronary artery remodelling and ischemia from FFRCT
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Sellers, Stephanie L., Fonte, Tim A., Grover, Rominder, Mooney, John, Weir-McCall, Jonathan, Lau, Karen PL., Chavda, Anesh, McNabney, Charis, Ahmadi, Amir, Blanke, Philipp, Payne, Geoffrey W., Murphy, Darra T., Ong, Kevin, Taylor, Charles A., and Leipsic, Jonathon A.
- Published
- 2018
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6. Neovascularization in Structural Bioprosthetic Valve Dysfunction
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Yoon, Joshua, Jelisejevas, Julius, Meier, David, Gill, Hacina, Lai, Althea, Seidman, Michael A., Payne, Geoffrey W., Cheung, Anson, Wood, David A., Leipsic, Jonathon A., Webb, John G., Sathananthan, Janarthanan, and Sellers, Stephanie L.
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- 2023
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7. Multimodality Imaging to Assess Leaflet Height in Mitral Bioprosthetic Valves: Implications for Mitral Valve-in-Valve Procedure
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Akodad, Mariama, Sathananthan, Janarthanan, Tzimas, Georgios, Salcudean, Hannah, Hensey, Mark, Gulsin, Gaurav S., Meier, David, (Anthony) Chuang, Ming-yu, Chatfield, Andrew G., Landes, Uri, Blanke, Philipp, Sondergaard, Lars, Payne, Geoffrey W., Lutter, Georg, Puehler, Thomas, Wood, David A., Webb, John G., Leipsic, Jonathon A., and Sellers, Stephanie L.
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- 2022
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8. CD4⁺ T cells support cytotoxic T lymphocyte priming by controlling lymph node input
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Kumamoto, Yosuke, Mattei, Lisa M., Sellers, Stephanie, Payne, Geoffrey W., and Iwasaki, Akiko
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- 2011
9. Abolition of arteriolar dilation but not constriction to histamine in cremaster muscle of eNO[S.sup.-/-] mice
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Payne, Geoffrey W., Madri, Joseph A., Sessa, William C., and Segal, Steven S.
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Blood flow -- Research ,Biological sciences - Abstract
Histamine increases the permeability of capillaries and venules but little is known of its precapillary actions on the control of tissue perfusion. Using gene ablation and pharmacological interventions, we tested whether histamine could increase muscle blood flow through stimulating nitric oxide (NO) release from microvascular endothelium. Vasomotor responses to topical histamine were investigated in second-order arterioles in the superfused cremaster muscle of anesthetized C57BL6 mice and null platelet endothelial cell adhesion molecule-1 (PECAM-[1.sup.-/-]) and null endothelial NO synthase ([eNOS.sup.-/-] ) mice aged 8-12 wk. Neither resting (17 [+ or -] [micro]m) nor maximum diameters (36 [+ or -] 2 [micro]m) were different between groups, nor was the constrictor response (~5 [+ or -] 1 [micro]m) to elevating superfusate oxygen from 0 to 21%. For arterioles of C57BL6 and PECAM-[1.sup.-/-] mice, cumulative addition of histamine to the superfusate produced vasodilation (1 nM-1 [micro]M; peak response, 9 [+ or -] I [micro]m) and then vasoconstriction (10-100 [micro]M; peak response, 12 [+ or -] 2 [micro]m). In [eNOS.sup.-/-] mice, histamine produced only vasoconstriction. In C57BL6 and PECAM-[1.sup.-/-] mice, vasodilation was abolished with [N.sup.[omega]]-nitro-L-arginine (30 [micro]M); in all mice, vasoconstriction was abolished with nifedipine (1 [micro]M). Vasomotor responses were eliminated with pyrilamine (1 [micro]M; [H.sub.1] receptor antagonist) yet remained intact with cimetidine (1 [micro]M; [H.sub.2] receptor antagonist). These findings illustrate that the biphasic vasomotor response of mouse cremaster arterioles to histamine is mediated through [H.sub.1] receptors on endothelium (NO-dependent vasodilation) as well as smooth muscle ([Ca.sup.2+] entry and constriction). Thus histamine can increase as well as decrease muscle blood flow, according to local concentration. However, when NO production is compromised, only vasoconstriction and flow reduction occur. microcirculation; blood flow control; endothelial nitric oxide synthase
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- 2003
10. Arteriolar network architecture and vasomotor function with ageing in mouse gluteus maximus muscle
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Bearden, Shawn E., Payne, Geoffrey W., Chisty, Alia, and Segal, Steven S.
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- 2004
11. Alterations in Autoregulatory and Myogenic Function in the Cerebrovasculature of Dahl Salt-Sensitive Rats
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Smeda, John S. and Payne, Geoffrey W.
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- 2003
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12. Impact of Bioprosthetic Valve Fracture on Potential Embolic Debris Generation: Insights From the Bench.
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Meier, David, Sreedharan, Subhashaan, Akodad, Mariama, Salcudean, Hannah, Lai, Althea, Chatfield, Andrew G., Ye, Jian, Cheung, Anson, Payne, Geoffrey W., Allen, Keith B., Chhatriwalla, Adnan K., Wood, David A., Webb, John G., Leipsic, Jonathon A., Sathananthan, Janarthanan, and Sellers, Stephanie L.
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- 2022
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13. Rhesus D factor (RhD) negative women's experiences with pregnancy: An interpretive description.
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Fyfe, Trina M., Lavoie, Josée G., Payne, Geoffrey W., and Banner, Davina
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The development of rh immune globulin (RhIG) for the prevention of Rhesus D (RhD) alloimmunization has significantly decreased the incidence of RhD alloimmunization. Despite long-standing prevention, the experiences of RhD negative women with pregnancy is absent in the literature. The purpose of this study was to explore the experiences of RhD negative women with pregnancy. Utilizing an Interpretive Description approach, semi-structured interviews were conducted with RhD negative women about their pregnancies. This study took place within the geographic context of northern British Columbia (BC). The analysis involved a two-cycle approach to identify themes within the data. Sixteen RhD negative women that live in northern BC participated in this study. The analysis identified that RhD negative women are uninformed and want to be involved in the decision-making process regarding the prevention of RhD alloimmunization. The themes that emerged from the interview data were communication, information-seeking behaviour, out of sight out of mind, choice and trust, and patient advocacy. The participants in this study described lacking information regarding the prevention of RhD alloimmunization. They sought information to overcome the gaps in knowledge and a desire to be involved in the decision-making process. RhD negative women want information and to be involved in the decision-making process in the prevention of RhD alloimmunization. Working with RhD negative women to develop decision-aids and/or other educational tools to aid in the decision-making process are warranted. [ABSTRACT FROM AUTHOR]
- Published
- 2020
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14. Impact of sublingual nitroglycerin dosage on FFRCT assessment and coronary luminal volume-to-myocardial mass ratio.
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Holmes, Kenneth R., Fonte, Tim A., Weir-McCall, Jonathan, Anastasius, Malcolm, Blanke, Philipp, Payne, Geoffrey W., Ellis, Jen, Murphy, Darra T., Taylor, Charles, Leipsic, Jonathon A., and Sellers, Stephanie L.
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NITROGLYCERIN ,WILCOXON signed-rank test ,HYPEREMIA ,DRUG dosage ,CORONARY vasospasm ,COMPUTED tomography ,CORONARY arteries - Abstract
Objectives: Fractional flow reserve computed tomography (FFRCT) depends upon nitroglycerin (NTG) inducing maximal hyperemia. However, the impact of NTG dosages on FFRCT analysis including coronary volume-to-mass ratio (V/M) is unknown.Methods: Eighty patients with repeat coronary CT angiograms (CCTAs) with different sublingual spray NTG doses (0.4 mg and 0.8 mg) were retrospectively analyzed with 45 patients excluded. Patient and scan demographics, post-stenosis and nadir FFRCT values, coronary volume, and coronary volume-to-mass ratio (V/M) were compared at initial CCTA (0.4 mg NTG) and follow-up CCTA (0.8 mg NTG). Differences were compared by Wilcoxon signed-rank test.Results: Thirty-five patients were included (time between CCTAs, 3.9 ± 1.6 years). Segment involvement score was 2.4 ± 3.3 and 2.8 ± 3.4 at initial and repeat CCTA (0.4 and 0.8 mg NTG), respectively (p = 0.004). There was similar image quality (4.1 ± 0.7 vs 4.1 ± 0.8; p = 0.51). Nadir FFRCT values did not differ in the left (0.4 mg, 0.80 ± 0.08 vs 0.8 mg, 0.80 ± 0.03; p = 0.66), right (0.4 mg, 0.90 ± 0.04 vs 0.8 mg, 0.90 ± 0.06; p = 0.25), or circumflex coronaries (0.4 mg, 0.87 ± 0.06 vs 0.8 mg, 0.88 ± 0.06; p = 0.34). Post-stenosis FFRCT values did not differ (p = 0.65). Coronary volume increased with 0.8 mg of NTG (2639 ± 753 mm3 vs 2844.8 ± 827 mm3; p = 0.009) but V/M ratio did not (p = 0.20).Conclusions: Use of 0.8 mg versus 0.4 mg of NTG in routine clinical CCTAs significantly increased coronary volume determined from FFRCT analysis but did not alter FFRCT or V/M. Further evaluation of repeat CCTAs in a more contemporaneous fashion using varied nitrate doses and disease severity is needed.Key Points: • Fractional flow reserve from computed tomography (FFRCT) is a noninvasive method for evaluating the coronary arteries and relies on nitroglycerin (NTG) to induce coronary vasodilation, but the impact of different NTG dosages is unknown. • Retrospective analysis evaluated use of different NTG doses on FFRCT. • Increased NTG dose increased coronary luminal volume on FFRCTanalysis, but did not change FFRCTvalues. [ABSTRACT FROM AUTHOR]- Published
- 2019
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15. Inonotus obliquus attenuates histamine-induced microvascular inflammation.
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Javed, Sumreen, Mitchell, Kevin, Sidsworth, Danielle, Sellers, Stephanie L., Reutens-Hernandez, Jennifer, Massicotte, Hugues B., Egger, Keith N., Lee, Chow H., and Payne, Geoffrey W.
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ENDOTHELIUM ,MAST cells ,ANTIHISTAMINES ,CONNECTIVE tissue cells ,VASCULAR endothelium ,GLUTEAL muscles - Abstract
Cell-to-cell communication is a key element of microvascular blood flow control, including rapidly carrying signals through the vascular endothelium in response to local stimuli. This cell-to-cell communication is negatively impacted during inflammation through the disruption of junctional integrity. Such disruption is associated with promoting the onset of cardiovascular diseases as a result of altered microvascular blood flow regulation. Therefore, understanding the mechanisms how inflammation drives microvascular dysfunction and compounds that mitigate such inflammation and dysfunction are of great interest for development. As such we aimed to investigate extracts of mushrooms as potential novel compounds. Using intravital microscopy, the medicinal mushroom, Inonotus obliquus was observed, to attenuate histamine-induced inflammation conducted vasodilation in second-order arterioles in the gluteus maximus muscle of C57BL/6 mice. Mast cell activation by C48/80 similarly disrupted endothelial junctions and conducted vasodilation but only histamine was blocked by the histamine antagonist, pyrilamine not C48/80 suggesting the importance of mast cell activation. Data presented here supports that histamine induced inflammation is a major disruptor of junctional integrity, and highlights the important anti-inflammatory properties of Inonotus obliquus focusing future assessment of mast cells as putative target for Inonotus obliquus. [ABSTRACT FROM AUTHOR]
- Published
- 2019
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16. Transcatheter Aortic Heart Valves: Histological Analysis Providing Insight to Leaflet Thickening and Structural Valve Degeneration.
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Sellers, Stephanie L., Turner, Christopher T., Sathananthan, Janarthanan, Cartlidge, Timothy R.G., Sin, Frances, Bouchareb, Rihab, Mooney, John, Nørgaard, Bjarne L., Bax, Jeroen J., Bernatchez, Pascal N., Dweck, Marc R., Granville, David J., Newby, David E., Lauck, Sandra, Webb, John G., Payne, Geoffrey W., Pibarot, Philippe, Blanke, Philipp, Seidman, Michael A., and Leipsic, Jonathon A.
- Abstract
Abstract Objectives This study investigated processes causing leaflet thickening and structural valve degeneration (SVD). Background Although transcatheter aortic valve replacement (TAVR) has changed the treatment of aortic stenosis, concerns remain regarding SVD, potentially related to valve thrombosis and thickening, based on studies using computed tomography (CT). Detailed histological analyses are provided to help attain insights into these processes. Methods Explanted transcatheter heart valves (THVs) were evaluated for thrombosis, fibrosis, and calcification for quantification of leaflet thickness. Immunohistochemical and microscopy approaches were used to investigate SVD-associated mechanisms. Results THVs (n = 23) were obtained from 22 patients (median 81 years of age; 50% male) from 0 to 2,583 days post TAVR. Maximal leaflet thickness increased relative to implant duration (ρ = 0.427; p = 0.027). THVs explanted after >2 years were thicker than those explanted after <2 years (p = 0.007). All THVs had adherent thrombus on both aortic and ventricular sides, which beyond 60 days was seen in combination with fibrosis and beyond 4 years had calcification. Early thrombus formation (<60 days) occurred despite rapid endothelialization with an abnormal hyperplastic phenotype. Fibrosis was observed in 6 patients on both the aortic and the ventricular THV surfaces, remodeled over time, and was associated with matrix metalloproteinase-1 expression. Five THVs showed overt calcification associated with adherent thrombus and fibrosis. Conclusions There is a time-dependent degeneration of THVs consisting of thrombus formation, endothelial hyperplasia, fibrosis, tissue remodeling, proteinase expression, and calcification. Future investigation is needed to further understand these mechanisms contributing to leaflet thickening and SVD. Graphical abstract [ABSTRACT FROM AUTHOR]
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- 2019
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17. Tricuspid Valve-in-Valve and Bioprosthetic Surgical Tricuspid and Pulmonic Valve Degeneration: Lessons From Imaging and Histopathology.
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Sellers, Stephanie L., Hensey, Mark, Cartlidge, Timothy R.G., Turner, Christopher T., Lau, Karen, Lai, Althea, Salcudean, Hannah, Sathananthan, Janarthanan, McManus, Bruce M., Granville, David J., Payne, Geoffrey W., Pibarot, Philippe, Webb, John G., Newby, David E., Blanke, Philipp, Seidman, Michael A., Dweck, Marc R., and Leipsic, Jonathon A.
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- 2020
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18. Nitric Oxide and TNFα Are Critical Regulators of Reversible Lymph Node Vascular Remodeling and Adaptive Immune Response.
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Sellers, Stephanie L., Iwasaki, Akiko, and Payne, Geoffrey W.
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TUMOR necrosis factor receptors ,NITRIC oxide ,LYMPH node physiology ,IMMUNE response ,MOLECULAR biology ,HERPES simplex ,CELLULAR signal transduction ,SEXUALLY transmitted diseases - Abstract
Lymph node (LN) vascular growth, at the level of the main arteriole, was recently characterized for the first time during infection. Arteriole diameter was shown to increase for at least seven days and to occur via a CD4
+ T cell dependent mechanism, with vascular expansion playing a critical role in regulating induction of adaptive immune response. Here, using intravital microscopy of the inguinal LN during herpes simplex type II (HSV-2) infection, the data provides the first studies that demonstrate arteriole expansion during infection is a reversible vascular event that occurs via eutrophic outward remodeling. Furthermore, using genetic ablation models, and pharmacological blockade, we reveal arteriole remodeling and LN hypertrophy to be dependent upon both endothelial nitric oxide synthase (eNOS) and TNFα expression. Additionally, we reveal transient changes in nitric oxide (NO) levels to be a notable feature of response to viral infection and LN vascular remodeling and provide evidence that mast cells are the critical source of TNFα required to drive arteriole remodeling. Overall, this study is the first to fully characterize LN arteriole vascular changes throughout the course of infection. It effectively reveals a novel role for NO and TNFα in LN cellularity and changes in LN vascularity, which represent key advances in understanding LN vascular physiology and adaptive immune response. [ABSTRACT FROM AUTHOR]- Published
- 2013
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19. Problem Based Learning and Evidence Based Medicine: Utilizing the Librarian.
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Fyfe, Trina M. and Payne, Geoffrey W.
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PROBLEM-based learning ,EVIDENCE-based medicine ,LIBRARY reference services - Abstract
The article discusses librarian involvement with problem based learning (PBL) and evidence based medicine (EMB), adapted from the paper "Undergraduate medical education: redefining the role of the librarian," by T.M. Fyfe and G.W. Payne, published in the International Congress on Medical Librarianship (ICML) 2009 Conference proceedings.
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- 2011
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20. CD4+ T cells support cytotoxic T lymphocyte priming by controlling lymph node input.
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Kumamoto, Yosuke, Mattei, Lisa M., Sellers, Stephanie, Payne, Geoffrey W., and Iwasaki, Akiko
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LYMPHOCYTES ,DENDRITIC cells ,IMMUNOLOGY ,LYMPHOID tissue ,IMMUNE response - Abstract
Rapid induction of CD8
+ cytotoxic T lymphocyte (CTL) responses is critical to combat acute infection with intracellular pathogens. CD4+ T cells help prime antigen-specific CTLs in secondary lymphoid organs after infection in the periphery. Although the frequency of naïve precursors is very low, the immune system is able to efficiently screen for cognate CTLs through mechanisms that are not well understood. Here we examine the role of CD4+ T cells in early phases of the immune response. We show that CD4+ T cells help optimal CTL expansion by facilitating entry of naïve polyclonal CD8+ T cells into the draining lymph node (dLN) early after infection or immunization. CD4+ T cells also facilitate input of naïve B cells into reactive LNs. Such "help" involves expansion of the arteriole feeding the dLN and enlargement of the dLN through activation of dendritic cells. In an antigen and CD40-dependent manner, CD4+ T cells activate dendritic cells to support naïve lymphocyte recruitment to the dLN. Our results reveal a previously unappreciated mode of CD4+ T-cell help, whereby they increase the input of naïve lymphocytes to the relevant LN for efficient screening of cognate CD8+ T cells. [ABSTRACT FROM AUTHOR]- Published
- 2011
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21. Effect of Inflammation on the Aging Microcirculation: Impact on Skeletal Muscle Blood Flow Control.
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Payne, Geoffrey W.
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- *
MICROCIRCULATION , *INFLAMMATION , *BLOOD flow , *CARDIOVASCULAR diseases , *AGING , *BLOOD vessels - Abstract
To meet the metabolic demands of skeletal muscle, the vasculature supplying these vascular beds has to be connected to respond in a coordinated uniform manner, thus providing the necessary oxygen and nutrients during increased activity. The skeletal muscle microcirculation is the major resistance network controlling vascular blood supply and it is the integrity of the endothelium lining the blood vessels that is paramount in facilitating this action. Aging is a major risk factor for cardiovascular disease and is associated with significant increases in inflammatory agents that negatively impact the vasculature. Several inflammatory agents such as cytokines (tumor necrosis factor-a), advanced glycation products (AGEs), and matrix metalloproteinases (MMPs) along with storage cells for inflammatory mediators (mast cells) are associated with a chronic “low-grade inflammation” state that has been observed over the course of the aging process. Current research suggests that these age-related increases in inflammatory agents can disrupt the microvascular endothelium and thus impair blood flow. This impairment could exacerbate the common age-related disease states such as hypertension, diabetes, congestive heart failure, and sarcopenia, leading to increased mortality and morbidity. [ABSTRACT FROM AUTHOR]
- Published
- 2006
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22. Innate control of adaptive immunity via remodeling of lymph node feed arteriole.
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Soderberg, Kelly A., Payne, Geoffrey W., Sato, Ayuko, Medzhitov, Ruslan, Segal, Steven S., and Iwasaki, Akiko
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- *
LYMPHOCYTES , *IMMUNITY , *IMMUNOGLOBULINS , *IMMUNE response , *LYMPH nodes , *IMMUNE system - Abstract
The adaptive immune system relies on rare cognate lymphocytes to detect pathogen-derived antigens. Naïve lymphocytes recirculate through secondary lymphoid organs in search of cognate antigen. Here, we show that the naïve-lymphocyte recirculation pattern is controlled at the level of innate immune recognition, independent of antigen-specific stimulation. We demonstrate that inflammation-induced lymphocyte recruitment to the lymph node is mediated by the remodeling of the primary feed arteriole, and that its physiological role is to increase the efficiency of screening for rare antigen-specific lymphocytes. Our data reveal a mechanism of innate control of adaptive immunity: by increasing the pool of naïve lymphocytes for detection of foreign antigens via regulation of vascular input to the local lymph node. [ABSTRACT FROM AUTHOR]
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- 2005
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23. Connexin expression and conducted vasodilation along arteriolar endothelium in mouse skeletal muscle.
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Looft-Wilson, Robin C., Payne, Geoffrey W., and Sega, Steven S.
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HYPEREMIA ,EXERCISE ,PHYSIOLOGY ,HEALTH ,MUSCLES ,EPITHELIUM - Abstract
Functional hyperemia requires the coordination of smooth muscle cell relaxation along and between branches of the arteriolar network. Vasodilation is conducted from cell to cell along the arteriolar wall through gap junction channels composed of connexin protein subunits. Within skeletal muscle, it is unclear whether arteriolar endothelium, smooth muscle, or both cell layers provide the cellular pathway for conduction. Furthermore, the constitutive profile of connexin expression within the microcirculation is unknown. We tested the hypothesis that conducted vasodilation and connexin expression are intrinsic to the endothelium of arterioles (17 ± 1 µm diameter) that supply the skeletal muscle fibers in the cremaster of anesthetized C57BL/6 mice. ACh delivered to an arteriole (500 ms, 1-µA pulse; 1-µm micropipette) produced local dilation of 17 ± 1 µm; conducted vasodilation observed 1 mm upstream was 9 ± 1 µm (n = 5). After light-dye treatment to selectively disrupt endothelium (250-µm segment centered 500 µm upstream, confirmed by loss of local response to ACh while constriction to phenylephrine and dilation to sodium nitroprusside remained intact), we found that conducted vasodilation was nearly abolished (2 ± 1 µm; P < 0.05). Whole-mount immunohistochemistry for connexins revealed punctate labeling at borders of arteriolar endothelial cells, with connexin40 and connexin37 in all branches and connexin43 only in the largest branches. Immunoreactivity for connexins was not apparent in smooth muscle or in capillary or venular endothelium, despite robust immunolabeling for α-actin and platelet endothelial cell adhesion molecule-1, respectively. We conclude that vasodilation is conducted along the endothelium of mouse skeletal muscle arterioles and that connexin40 and connexin37 are the primary connexins forming gap junction channels between arteriolar endothelial cells. [ABSTRACT FROM AUTHOR]
- Published
- 2004
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24. Histamine inhibits conducted vasodilation through endothelium-derived NO production in arterioles of mouse skeletal muscle.
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Payne, Geoffrey W., Madri, Joseph A., Sessa, William C., and Segal, Steven S.
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- *
VASODILATION , *ENDOTHELIUM , *HISTAMINE , *GAP junctions (Cell biology) , *CELL junctions - Abstract
Conducted vasodilation along arterioles manifests the spread of hyperpolarization through gap junction channels along endothelium. Whereas histamine increases the permeability of capillary and venular endothelium, its effect on the integrity of arteriolar endothelium is unknown. We tested whether histamine could inhibit conducted vasodilation. In second-order arterioles (2A) supplying the cremaster muscle of C57BL6, PECAM-1-/-, and eNOS-/- mice (8-12 wk), neither resting (16 ± 2 µm) nor maximal (38 ± 2 µm) diameters were different. Acetylcholine (ACh) microiontophoresis (1 µA, 500 ms pulse) triggered vasodilation that was conducted > 1400 µm along arterioles. Neither local (14 ± 2 µm) nor conducted vasodilation (10 ± 2 µm) was different among mice. Histamine (5 µM) had no effect on resting diameter or local vasodilation to ACh yet inhibited conduction by > 50% in C57BL6 and PECAM-1-/- mice (P < 0.05); this effect was abolished after blockade of NO synthase or of soluble guanylate cyclase. Washout of histamine restored conduction, though recovery was longer (P < 0.05) in PECAM-1-/- mice vs. C57BL6 mice. Remarkably, conducted vasodilation in eNOS-/- mice was insensitive to histamine. These findings indicate that histamine inhibits cell-to-cell coupling through an NO-dependent mechanism and suggests a dynamic interaction among intercellular adhesion molecules and gap junction channels along arteriolar endothelium. [ABSTRACT FROM AUTHOR]
- Published
- 2004
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25. Effects of hypomagnesia on histamine H1 receptor-mediated facilitation of NMDA responses.
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Payne, Geoffrey W and Neuman, Richard S
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- 1997
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26. The Microcirculation of Skeletal Muscle in Aging.
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Payne, Geoffrey W. and Bearden, Shawn W.
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- *
MICROCIRCULATION , *NERVOUS system , *AGING , *SYMPATHETIC nervous system , *ORGANS (Anatomy) , *BLOOD flow - Abstract
Microvascular structure and function are key aspects of tissue and organ health. At approximately 40% of total body mass, skeletal muscle contains more microvessels than any other organ system in the body. Moreover, skeletal muscle is the most dynamic tissue in the body with the capacity to increase blood flow and metabolic rate 30- to 50- fold. Aging is associated with decrements in microvascular function and exercise tolerance that are poorly understood. Here, experts in their respective fields of microvascular structure and function are brought together to review the current state of knowledge regarding microvascular adaptations to aging. Reviews are drawn from human and animal studies and focus on age-related changes in sympathetic nervous system control of microvessels, capillary hemodynamics and oxygen pressure, microvascular network structure and functional integration, microvascular reactivity, whole muscle perfusion, and cellular contacts and inflammation. [ABSTRACT FROM AUTHOR]
- Published
- 2006
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27. Anti-Inflammatory Activity of the Wild Mushroom, Echinodontium tinctorium, in RAW264.7 Macrophage Cells and Mouse Microcirculation.
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Javed, Sumreen, Li, Wai Ming, Zeb, Mehreen, Yaqoob, Almas, Tackaberry, Linda E., Massicotte, Hugues B., Egger, Keith N., Cheung, Peter C.K., Payne, Geoffrey W., Lee, Chow H., and Miguel, Maria da Graça Costa G.
- Subjects
POLYSACCHARIDES ,MICROCIRCULATION ,MUSHROOMS ,GLUTEAL muscles ,GLUCANS ,MOLECULAR weights ,MICE ,BETA-glucans - Abstract
The aim of this study was to investigate the anti-inflammatory activity of a previously un-studied wild mushroom, Echinodontium tinctorium, collected from the forests of north-central British Columbia. The lipopolysaccharide (LPS)-induced RAW264.7 macrophage model was used to study the in vitro anti-inflammatory activity. The crude alkaline extract demonstrated potent anti-inflammatory activity, and was further purified using a "bio-activity-guided-purification" approach. The size-exclusion and ion-exchange chromatography yielded a water-soluble anti-inflammatory polysaccharide (AIPetinc). AIPetinc has an average molecular weight of 5 kDa, and is a heteroglucan composed of mainly glucose (88.6%) with a small amount of galactose (4.0%), mannose (4.4%), fucose (0.7%), and xylose (2.3%). In in vivo settings, AIPetinc restored the histamine-induced inflammatory event in mouse gluteus maximus muscle, thus confirming its anti-inflammatory activity in an animal model. This study constitutes the first report on the bioactivity of Echinodontium tinctorium, and highlights the potential medicinal benefits of fungi from the wild forests of northern British Columbia. Furthermore, it also reiterates the need to explore natural resources for alternative treatment to modern world diseases. [ABSTRACT FROM AUTHOR]
- Published
- 2019
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28. Problem-based learning tutors within medical curricula: An interprofessional analysis.
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Gingerich, Andrea, Mader, Heidi, and Payne, Geoffrey W.
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CURRICULUM evaluation ,ANALYSIS of variance ,COLLEGE teachers ,INTERDISCIPLINARY education ,PROBABILITY theory ,PROBLEM-based learning ,RESEARCH funding ,STATISTICS ,DATA analysis ,QUANTITATIVE research ,DESCRIPTIVE statistics - Abstract
The article presents a study regarding the use of non-health professionals as problem-based learning (PBL) tutors in an undergraduate medical program. The study used the anonymized student academic records, PBL groupings, and tutor evaluations obtained from the University of British Columbia's (UBC's) Northern Medical Program (NMP). Results showed that non-health professionals can be used as PBL tutors without negatively impacting student achievement on written examinations.
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- 2012
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29. Impact of Smoking on Coronary Volume-to-Myocardial Mass Ratio: An ADVANCE Registry Substudy.
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Holmes KR, Gulsin GS, Fairbairn TA, Hurwitz-Koweek L, Matsuo H, Nørgaard BL, Jensen JM, Sand NR, Nieman K, Bax JJ, Pontone G, Chinnaiyan KM, Rabbat MG, Amano T, Kawasaki T, Akasaka T, Kitabata H, Rogers C, Patel MR, Payne GW, Leipsic JA, and Sellers SL
- Subjects
- Female, Humans, Male, Coronary Angiography, Heart, Myocardium, Smoking adverse effects, Coronary Artery Disease diagnostic imaging, Fractional Flow Reserve, Myocardial
- Abstract
Purpose To examine the relationship between smoking status and coronary volume-to-myocardial mass ratio (V/M) among individuals with coronary artery disease (CAD) undergoing CT fractional flow reserve (CT-FFR) analysis. Materials and Methods In this secondary analysis, participants from the ADVANCE registry evaluated for suspected CAD from July 15, 2015, to October 20, 2017, who were found to have coronary stenosis of 30% or greater at coronary CT angiography (CCTA) were included if they had known smoking status and underwent CT-FFR and V/M analysis. CCTA images were segmented to calculate coronary volume and myocardial mass. V/M was compared between smoking groups, and predictors of low V/M were determined. Results The sample for analysis included 503 current smokers, 1060 former smokers, and 1311 never-smokers (2874 participants; 1906 male participants). After adjustment for demographic and clinical factors, former smokers had greater coronary volume than never-smokers (former smokers, 3021.7 mm
3 ± 934.0 [SD]; never-smokers, 2967.6 mm3 ± 978.0; P = .002), while current smokers had increased myocardial mass compared with never-smokers (current smokers, 127.8 g ± 32.9; never-smokers, 118.0 g ± 32.5; P = .02). However, both current and former smokers had lower V/M than never-smokers (current smokers, 24.1 mm3 /g ± 7.9; former smokers, 24.9 mm3 /g ± 7.1; never-smokers, 25.8 mm3 /g ± 7.4; P < .001 [unadjusted] and P = .002 [unadjusted], respectively). Current smoking status (odds ratio [OR], 0.74 [95% CI: 0.59, 0.93]; P = .009), former smoking status (OR, 0.81 [95% CI: 0.68, 0.97]; P = .02), stenosis of 50% or greater (OR, 0.62 [95% CI: 0.52, 0.74]; P < .001), and diabetes (OR, 0.67 [95% CI: 0.56, 0.82]; P < .001) were independent predictors of low V/M. Conclusion Both current and former smoking status were independently associated with low V/M. Keywords: CT Angiography, Cardiac, Heart, Ischemia/Infarction Clinical trial registration no. NCT02499679 Supplemental material is available for this article . © RSNA, 2024.- Published
- 2024
- Full Text
- View/download PDF
30. Redo-TAVI with SAPIEN 3 in SAPIEN XT or SAPIEN 3 - impact of pre- and post-dilatation on final THV expansion.
- Author
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Meier D, Landes U, Sondergaard L, De Backer O, Lutter G, Puehler T, Akodad M, Tzimas G, Blanke P, Payne GW, Lai A, Gill H, Wood DA, Webb JG, Sellers SL, and Sathananthan J
- Subjects
- Humans, X-Ray Microtomography, Dilatation, Treatment Outcome, Aortic Valve diagnostic imaging, Aortic Valve surgery, Prosthesis Design, Transcatheter Aortic Valve Replacement methods, Aortic Valve Insufficiency surgery, Aortic Valve Stenosis diagnostic imaging, Aortic Valve Stenosis surgery, Heart Valve Prosthesis
- Abstract
Background: When a balloon-expandable transcatheter heart valve (THV) is chosen to treat a failed balloon-expandable THV, there is a risk of underexpansion with a potential impact on performance., Aims: We aimed to assess the impact of pre- and post-dilatation on the expansion of balloon-expandable THVs after redo-transcatheter aortic valve implantation (TAVI)., Methods: Redo-TAVI was performed on the bench with a 23 mm SAPIEN 3 (S3) implanted within a 23 mm SAPIEN XT (SXT) or a 23 mm S3, both of which served as the "failed" THVs. Pre- and/or post-dilatation was performed using a 23 mm non-compliant TRUE balloon. Expansion of the index and redo-THVs were assessed before and after pre-/post-dilatation using microcomputed tomography (micro-CT), and THV hydrodynamic testing was conducted., Results: Without pre- or post-dilatation, the S3 was underexpanded, for all combinations, particularly in the mid-portion of the THV (18.6 mm and 19.7 mm representing 81% and 86% of the nominal diameter inside the SXT and S3, respectively). Pre- and post-dilatation had an additive effect on diameter expansion of the redo-THV, which remained constrained in most combinations. The only combination to achieve nominal expansion was the S3 in S3 when both pre- and post-dilatation were performed. The S3 remained underexpanded inside the SXT despite pre- and post-dilatation (93% in the mid-portion). Improved redo-THV expansion was accompanied by 2.7 mm (12%) overexpansion of the index THV. While all samples had acceptable hydrodynamic performance, the underexpanded samples had worse leaflet pinwheeling., Conclusions: When performing redo-TAVI with a 23 mm S3 inside a 23 mm SXT or S3, only the S3 in S3 with the use of pre- and post-dilatation reached full expansion. This underlines the importance of CT assessment of THV expansion and the role of pre-/post-dilatation.
- Published
- 2023
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- View/download PDF
31. Timing of bioprosthetic valve fracture in transcatheter valve-in-valve intervention: impact on valve durability and leaflet integrity.
- Author
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Meier D, Payne GW, Mostaço-Guidolin LB, Bouchareb R, Rich C, Lai A, Chatfield AG, Akodad M, Salcudean H, Lutter G, Puehler T, Pibarot P, Allen KB, Chhatriwalla AK, Sondergaard L, Wood DA, Webb JG, Leipsic JA, Sathananthan J, and Sellers SL
- Subjects
- Humans, Prosthesis Design, Aortic Valve surgery, Treatment Outcome, Transcatheter Aortic Valve Replacement, Heart Valve Prosthesis, Bioprosthesis, Aortic Valve Stenosis surgery
- Abstract
Background: Bioprosthetic valve fracture (BVF) can be used to improve transcatheter heart valve (THV) haemodynamics following a valve-in-valve (ViV) intervention. However, whether BVF should be performed before or after THV deployment and the implications on durability are unknown. Aims: We sought to assess the impact of BVF timing on long-term THV durability., Methods: The impact of BVF timing was assessed using small ACURATE neo (ACn) or 23 mm SAPIEN 3 (S3) THV deployed in 21 mm Mitroflow valves compared to no-BVF controls. Valves underwent accelerated wear testing up to 200 million (M) cycles (equivalent to 5 years). At 200M cycles, THV were evaluated by hydrodynamic testing, second-harmonic generation (SHG) microscopy, scanning electron microscopy (SEM) and histology., Results: At 200M cycles, the regurgitant fraction (RF) and effective orifice area (EOA) for the ACn were 8.03±0.30%/1.74±0.01 cm
2 (no BVF), 12.48±0.70%/1.97±0.02 cm2 (BVF before ViV) and 9.29±0.38%/2.21±0.0 cm2 (BVF after ViV), respectively. For the S3 these values were 2.63±0.51%/1.26±0.01 cm2 , 2.03±0.42%/1.65±0.01 cm2 , and 1.62±0.38%/2.22±0.01 cm2 , respectively. Further, SHG and SEM revealed a higher degree of superficial leaflet damage when BVF was performed after ViV for the ACn and S3. However, the histological analysis revealed significantly less damage, as determined by matrix density analysis, through the entire leaflet thickness when BVF was performed after ViV with the S3 and a similar but non-significant trend with the ACn. Conclusions: BVF performed after ViV appears to offer superior long-term EOA without increased RF. Ultrastructure leaflet analysis reveals that the timing of BVF can differentially impact leaflets, with more superficial damage but greater preservation of overall leaflet structure when BVF is performed after ViV.- Published
- 2023
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32. Rural healthcare delivery: Navigating a complex ecosystem.
- Author
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Fyfe TM and Payne GW
- Subjects
- British Columbia, Evidence-Based Practice, Female, Humans, Interviews as Topic, Maternal Health Services, Pregnancy, Qualitative Research, Rh Isoimmunization prevention & control, Rh-Hr Blood-Group System, Delivery of Health Care, Patient Navigation, Rural Health Services
- Abstract
Clinical Practice Guidelines (CPGs) provide evidence-based recommendations for Healthcare Providers (HCPs) to utilize when making patient care decisions. Rural providers face challenges in the provision of evidence-based care, including the use of guidelines. The aim of this article is to explore the complexities of providing healthcare in rural areas. This article will focus on a specific aspect of rural maternity care with well-established CPGs, the prevention of Rhesus D factor alloimmunization. An applied health research approach, interpretive description, utilized semistructured interviews with HCPs across the vast geographic region of northern British Columbia. The study found that HCPs are aware of guidelines but face various barriers during implementation. In order to implement guidelines within practice, rural HCPs adapt processes to overcome local barriers. These process adaptations need to be identified and shared across a large health authority with a complex geography and healthcare system to ensure quality of care.
- Published
- 2020
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33. The Authors Reply.
- Author
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Sellers SL, Payne GW, Seidman MA, and Leipsic JA
- Subjects
- Heart Valves
- Published
- 2019
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34. Modified Intravital Microscopy to Assess Vascular Health and T-Cell Motility.
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Payne GW, Mitchell K, and Sellers SL
- Subjects
- Animals, Cell Communication, Mice, Cell Movement, Cell Tracking methods, Intravital Microscopy methods, Lymph Nodes blood supply, Lymph Nodes immunology, Microcirculation, T-Lymphocytes immunology
- Abstract
The ability to study the microcirculation in real time is key to elucidating how the immune system and the associated microvasculature interact and influence one another within the lymph node (LN). Here, we present a method for near in-situ imaging of the inguinal LN. In particular, this method is ideal for the assessment of overall vascular health that influences immune functions and for the evaluation of T-cell motility. We focus on imaging of the microvasculature of the LN, paying particular attention to methods that ensure the study of healthy vessels, the ability to maintain imaging of viable vessels over a number of hours, quantification of vessel magnitude and vessel integrity. Modified intravital microscopy (M-IVM) of the LNs allows direct evaluation of microvascular functions as well as real-time imaging of the direct interface between immune cells, the LN, and the microcirculation. Importantly, M-IVM technique can be readily combined with many other vascular and immunological techniques such as fluorescent cell labeling and assessment of sticking and rolling time as descripted. Furthermore, it can be adapted to study vasculature of other than the inguinal LN. Overall, this chapter provides a dependable method for fundamental vascular immunological assessment of LNs that is decidedly useful in a diverse range of investigations.
- Published
- 2019
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- View/download PDF
35. Increased nonHDL cholesterol levels cause muscle wasting and ambulatory dysfunction in the mouse model of LGMD2B.
- Author
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Sellers SL, Milad N, White Z, Pascoe C, Chan R, Payne GW, Seow C, Rossi F, Seidman MA, and Bernatchez P
- Subjects
- Animals, Dysferlin deficiency, Female, Mice, Mice, Inbred C57BL, Mice, Knockout, Cholesterol metabolism, Disease Models, Animal, Dysferlin metabolism, Muscular Atrophy metabolism, Muscular Dystrophies, Limb-Girdle metabolism
- Abstract
Progressive limb and girdle muscle atrophy leading to loss of ambulation is a hallmark of dysferlinopathies, which include limb-girdle muscular dystrophy type 2B and Miyoshi myopathy. However, animal models fail to fully reproduce the disease severity observed in humans, with dysferlin-null (Dysf
-/- ) mice exhibiting minor muscle damage and weakness without dramatic ambulatory dysfunction. As we have previously reported significant Dysf expression in blood vessels, we investigated the role of vascular function in development of muscle pathology by generating a Dysf-deficient mouse model with vascular disease. This was achieved by crossing Dysf-/- mice with ApoE-/- mice, which have high levels of nonHDL-associated cholesterol. Double-knockout Dysf-/- ApoE-/- mice exhibited severe ambulatory dysfunction by 11 months of age. In limb-girdle muscles, histology confirmed dramatic muscle wasting, fibrofatty replacement, and myofiber damage in Dysf-/- ApoE-/- mice without affecting the ratio of centrally nucleated myofibers. Although there were no major changes in ex vivo diaphragm and soleus muscle function, histological analyses revealed these muscles to be untouched by damage and remodelling. In all, these data suggest that cholesterol may be deleterious to dysferlinopathic muscle and lead to ambulatory dysfunction. Moreover, differences in plasma lipid handling between mice and humans could be a key factor affecting dysferlinopathy severity., (Copyright © 2018 by the American Society for Biochemistry and Molecular Biology, Inc.)- Published
- 2018
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36. Growth-Inhibitory and Immunomodulatory Activities of Wild Mushrooms from North-Central British Columbia (Canada).
- Author
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Smith A, Javed S, Barad A, Myhre V, Li WM, Reimer K, Massicotte HB, Tackaberry LE, Payne GW, Egger KN, and Lee CH
- Subjects
- Animals, Ascomycota classification, Ascomycota genetics, Basidiomycota classification, Basidiomycota genetics, British Columbia, Cell Survival drug effects, HeLa Cells, Humans, Immunomodulation drug effects, Mice, RAW 264.7 Cells, Anti-Inflammatory Agents pharmacology, Ascomycota chemistry, Basidiomycota chemistry, Immunologic Factors pharmacology, Lipopolysaccharides pharmacology
- Abstract
Wild mushrooms, especially from North America, have not been systematically explored for their medicinal properties. Here we report screening for the growth-inhibitory and immunomodulatory activities of 12 species collected from multiple locations in north-central British Columbia, Canada. Mushrooms were characterized using morphology and DNA sequencing, followed by chemical extraction into 4 fractions using 80% ethanol, 50% methanol, water, and 5% sodium hydroxide. Growth-inhibitory, immunostimulatory, and anti-inflammatory activities of 5 mushrooms (Leucocybe connata, Trichaptum abietinum, Hydnellum sp., Gyromitra esculenta, and Hericium coralloides) are reported here, to our knowledge for the first time. Growth-inhibitory effects were assessed using the cytotoxic MTT assay. Immunostimulatory activity was assessed by tumor necrosis factor-α production in Raw 264.7 macrophages, whereas anti-inflammatory activity was assessed based on the inhibition of lipopolysaccharide-induced tumor necrosis factor-α production. The ethanol and aqueous extracts of Hydnellum sp. were potent growth inhibitors, with a half-maximal inhibitory concentration of 0.6 mg/mL. All 5 fungi displayed strong immunostimulatory activity, whereas only L. connata and T. abietinum showed strong anti-inflammatory activity. For the 7 other fungi investigated, which included well-known medicinal species such as Inonotus obliquus, Phellinus igniarius, and Ganoderma applanatum, the remarkable similarities in the biological activities reported here, and by others for specimens collected elsewhere, suggest that mushrooms can produce similar metabolites regardless of their habitat or ecosystem. This is to our knowledge the first study to explore wild mushrooms from British Columbia for biological activities that are relevant to cancer, and the results provide an initial framework for the selection of mushroom species with the potential for discovery of novel anticancer compounds.
- Published
- 2017
- Full Text
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37. Intravital microscopy of the inguinal lymph node.
- Author
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Sellers SL and Payne GW
- Subjects
- Acetylcholine pharmacology, Animals, Inguinal Canal, Lymph Nodes drug effects, Mice, Phenylephrine pharmacology, Lymph Nodes blood supply, Lymph Nodes immunology, Microscopy methods
- Abstract
Lymph nodes (LN's), located throughout the body, are an integral component of the immune system. They serve as a site for induction of adaptive immune response and therefore, the development of effector cells. As such, LNs are key to fighting invading pathogens and maintaining health. The choice of LN to study is dictated by accessibility and the desired model; the inguinal lymph node is well situated and easily supports studies of biologically relevant models of skin and genital mucosal infection. The inguinal LN, like all LNs, has an extensive microvascular network supplying it with blood. In general, this microvascular network includes the main feed arteriole of the LN that subsequently branches and feeds high endothelial venules (HEVs). HEVs are specialized for facilitating the trafficking of immune cells into the LN during both homeostasis and infection. How HEVs regulate trafficking into the LN under both of these circumstances is an area of intense exploration. The LN feed arteriole, has direct upstream influence on the HEVs and is the main supply of nutrients and cell rich blood into the LN. Furthermore, changes in the feed arteriole are implicated in facilitating induction of adaptive immune response. The LN microvasculature has obvious importance in maintaining an optimal blood supply to the LN and regulating immune cell influx into the LN, which are crucial elements in proper LN function and subsequently immune response. The ability to study the LN microvasculature in vivo is key to elucidating how the immune system and the microvasculature interact and influence one another within the LN. Here, we present a method for in vivo imaging of the inguinal lymph node. We focus on imaging of the microvasculature of the LN, paying particular attention to methods that ensure the study of healthy vessels, the ability to maintain imaging of viable vessels over a number of hours, and quantification of vessel magnitude. Methods for perfusion of the microvasculature with vasoactive drugs as well as the potential to trace and quantify cellular traffic are also presented. Intravital microscopy of the inguinal LN allows direct evaluation of microvascular functionality and real-time interface of the direct interface between immune cells, the LN, and the microcirculation. This technique potential to be combined with many immunological techniques and fluorescent cell labelling as well as manipulated to study vasculature of other LNs.
- Published
- 2011
- Full Text
- View/download PDF
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