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3 záznamů v Medvik

Článek

Kinematics of recreational male runners in "super", minimalist and habitual shoes

Hébert-Losier, Kim
Autor Hébert-Losier, Kim ORCID Division of Health, Engineering, Computing and Science, Te Huataki Waiora School of Health, University of Waikato, Tauranga, New Zealand Research & Development, The Running Clinic, Lac Beauport, Québec, Canada
Finlayson, Steven J
Autor Finlayson, Steven J Division of Health, Engineering, Computing and Science, Te Huataki Waiora School of Health, University of Waikato, Tauranga, New Zealand
Lamb, Peter F
Autor Lamb, Peter F ORCID School of Physical Education, Sport and Exercise Sciences, University of Otago, Dunedin, New Zealand
Driller, Matthew W
Autor Driller, Matthew W ORCID Sport and Exercise Science, School of Allied Health, Human Services and Sport, La Trobe University, Melbourne, Victoria, Australia
Hanzlíková, Ivana
Autor Hanzlíková, Ivana ORCID Department of Physiotherapy, Faculty of Physical Culture, Palacký University Olomouc, Olomouc, Czech Republic
Dubois, Blaise
Autor Dubois, Blaise ORCID Research & Development, The Running Clinic, Lac Beauport, Québec, Canada
Esculier, Jean-Francois
Autor Esculier, Jean-Francois ORCID Research & Development, The Running Clinic, Lac Beauport, Québec, Canada Department of Physical Therapy, University of British Columbia, Vancouver, British Columbia, Canada
Beaven, Christopher Martyn
Autor Beaven, Christopher Martyn ORCID Division of Health, Engineering, Computing and Science, Te Huataki Waiora School of Health, University of Waikato, Tauranga, New Zealand

Journal of sports sciences. 2022 ; 40 (13) : 1426-1435. [pub] 20220614

J Sports Sci
ISSN 1466-447X
Medvik
Zdroj

We conducted an exploratory analysis to compare running kinematics of 16 male recreational runners wearing Nike Vaporfly 4% (VP4), Saucony Endorphin racing flat (FLAT), and their habitual (OWN) footwear. We also explored potential relationships between kinematic and physiological changes. Runners (age: 33 ± 12 y, V ̇ O2peak: 55.2 ± 4.3 ml · kg-1·min-1) attended 3 sessions after completing an V ̇ O2peak test in which sagittal plane 3D kinematics at submaximal running speeds (60%, 70% and 80% ʋ V ̇ O2peak) were collected alongside economy measures. Kinematics were compared using notched boxplots, and between-shoe kinematic differences were plotted against between-shoe economy differences. Across intensities, VP4 involved longer flight times (6.7 to 10.0 ms) and lower stance hip range of motion (~3°), and greater vertical pelvis displacement than FLAT (~0.4 cm). Peak dorsiflexion angles (~2°), ankle range of motion (1.0° to 3.9°), and plantarflexion velocities (11.3 to 89.0 deg · sec-1) were greatest in FLAT and lowest in VP4. Foot-ground angles were smaller in FLAT (2.5° to 3.6°). Select kinematic variables were moderately related to economy, with higher step frequencies and shorter step lengths in VP4 and FLAT associated with improved economy versus OWN. Footwear changes from OWN altered running kinematics. The most pronounced differences were observed in ankle, spatiotemporal, and foot-ground angle variables.

Článek online

Histone H3.3G34-Mutant Interneuron Progenitors Co-opt PDGFRA for Gliomagenesis

Cell. 2020 ; 183 (6) : 1617-1633.e22. [pub] 20201130

ISSN 1097-4172
Medvik
Zdroj

Histone H3.3 glycine 34 to arginine/valine (G34R/V) mutations drive deadly gliomas and show exquisite regional and temporal specificity, suggesting a developmental context permissive to their effects. Here we show that 50% of G34R/V tumors (n = 95) bear activating PDGFRA mutations that display strong selection pressure at recurrence. Although considered gliomas, G34R/V tumors actually arise in GSX2/DLX-expressing interneuron progenitors, where G34R/V mutations impair neuronal differentiation. The lineage of origin may facilitate PDGFRA co-option through a chromatin loop connecting PDGFRA to GSX2 regulatory elements, promoting PDGFRA overexpression and mutation. At the single-cell level, G34R/V tumors harbor dual neuronal/astroglial identity and lack oligodendroglial programs, actively repressed by GSX2/DLX-mediated cell fate specification. G34R/V may become dispensable for tumor maintenance, whereas mutant-PDGFRA is potently oncogenic. Collectively, our results open novel research avenues in deadly tumors. G34R/V gliomas are neuronal malignancies where interneuron progenitors are stalled in differentiation by G34R/V mutations and malignant gliogenesis is promoted by co-option of a potentially targetable pathway, PDGFRA signaling.

Článek online

Guidelines for the use and interpretation of assays for monitoring autophagy (3rd edition)

Autophagy. 2016 ; 12 (1) : 1-222.

ISSN 1554-8635
Medvik
Zdroj

MeSH
autofagie * fyziologie MeSH
biotest metody normy MeSH
lidé MeSH
počítačová simulace MeSH
zvířata MeSH
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zvířata MeSH
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časopisecké články MeSH
Research Support, N.I.H., Extramural MeSH
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Hébert, Steven* Dotaz Zobrazit nápovědu

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