Your search keyword '"Kelly, Liam P."' showing total 57 results

51. Random harvest.

Author

Kelly, Liam

Abstract

The article offers information on the exhibition featuring the works of artist Siobhán Hapaska to be held at the Ormeau Baths Gallery (OBG) in Belfast, Northern Ireland on September 24, 2010.

Published

2010

52. Looking for Christmas decorations?

Author

Kelly, Liam

Abstract

The article presents information on Christmas decorations which can be found in garden centers. Traditional Christmas plants such as poinsettias, azaleas and kalanchoe can be found in garden centers. Most garden centers tend to stock items not found in other Christmas shops and people love it when they open their Christmas extravaganzas in October.

Published

2007

53. A growing movement!

Author

Kelly, Liam

Abstract

The article focuses on the increasing number of specialist nurseries in Ireland. There are several specialist nurseries in the country. These include the nursery owned by June Blake in Blessing. Another is the Mount Venus Nursery in Dublin, Ireland which is owned by Oliver and Liat Schurmann. In Wexford, Gerry Harford and Susan Carrick owned and run the Camolin Potting Shed. The plants and services offered at the nurseries are mentioned.

Published

2007

54. High Resolution Time-Lapse Monitoring of Individual Hematopoietic Stem Cells Reveals New Biomarkers of Self-Renewal.

Author

Dykstra, Brad, Ramunas, John, Kent, David, McCaffrey, Lindsay, Szumsky, Erin, Kelly, Liam, Farn, Kristin, Eaves, Connie, and Jervis, Eric

Abstract

Recently described strategies for isolating nearly pure populations of hematopoietic stem cells (HSCs) from normal adult mouse bone marrow (BM) offer new opportunities to identify previously unrecognized properties of HSCs Unfortunately, most phenotypic markers thus far found to characterize HSCs are not tightly linked to the functional potential of these cells but, instead, vary independently when their activation status is altered. Here we describe the results of experiments in which single CD45+Lin-Rho-SP adult mouse BM cells were micromanipulated into microwells of a specially designed silicone array and were monitored in real time (every 3 min) for a total of 4 days by high resolution digital time lapse photography to track the behavior of each cell and its clonal progeny. During this time, the cells were maintained at 37°C in a feeder-free, serum-free medium supplemented with 300 ng/mL SF, 20 ng/mL IL-11, and 1ng/mL Flt3-L. Under these conditions, 64 of 66 input cells divided at least once, and 63 divided at least twice. Only 2/715 cells tracked died. Final clones varied in size from 1-92 cells, corresponding to 0–7 cell cycles. The initial division occurred after 41±12 hr, and the 2nd and 3rd divisions another 18±5 and 16±4 hr later. Synchrony of sister cell divisions within clones and the presence of cells displaying uropodia (lagging protrusions) or lamellipodia (leading protrusions) were common. HSC activity in 83 initial CD45+Lin-Rho-SP cells or the 66 derived clones was assessed by transplanting these individually into sublethally irradiated Ly5-congenic W41/W41 recipients, which were then analyzed for longterm, multilineage, donor-derived WBCs (>1% @ 16 wk). 33% (27/83), of the initial cells were HSCs (producing 1–84% of WBCs @ 16 wk) and 27% (18/66) of the 4-day clones had HSC activity (2–83% of WBCs @ 16 wk), showing that many input HSCs had executed self-renewal divisions. Cells in clones containing HSCs had longer 1st, 2nd, and 3rd cycle times compared to cells within non-repopulating clones (5.4±2.3 hr, 3.7±1.0 hr, and 2.8±0.6 hr longer, respectively, p<.02 for each) and the cumulative time to the 3rd division was on average, 12±2 hr longer (p<.001) for cells in clones with HSCs. Similarly, clones containing HSCs underwent fewer divisions overall (3.2±0.2 vs 4.2±0.2, p=.003) and were therefore smaller (10±1 vs 26±3 cells, p<.001). All 24 clones in which >50% of cells had a cumulative time to their 3rd division of ≤ 65.3 hr (ie, < mean - 0.5 SD) lacked HSC activity. However, neither of the 2 cells that did not divide in the 4-day period were HSCs. The 22 clones in which all cells displayed uropodia within the final 12 hr of culture also lacked HSCs. Combined, these parameters allowed the 18 HSC-containing clones to be identified in a subset of 30 out of the original 66; ie, 2x more frequently. To test the validity of these parameters for predicting HSC-containing clones, a 2nd experiment was performed and similarly analyzed. In this case, these parameters identified 5 HSC-containing clones in a subset of 34 out of an original total of 76, again a 2-fold increase. These studies illustrate the potential of this novel monitoring system to detect new features of proliferating HSCs that are predictive of self-renewal events.

Published

2005

55. The big picture.

Author

Kelly, Liam

Abstract

The article previews the exhibition "Recent Paintings," featuring landscape paintings by Irish artist Clement McAleer, to be held at the Hamilton Gallery in Sligo, Ireland from November 1 to December 1, 2012.

Published

2012

56. Prior Band-Resisted Squat Jumps Improves Running and Neuromuscular Performance in Middle-Distance Runners.

Author

Low JL, Ahmadi H, Kelly LP, Willardson J, Boullosa D, and Behm DG

Subjects

Adult, Athletes, Electromyography, Humans, Isometric Contraction, Male, Muscle, Skeletal physiology, Posture, Athletic Performance physiology, Physical Endurance, Running physiology, Warm-Up Exercise

Abstract

Post-activation potentiation (PAP) conditioning has been reported to increase performance. Most research has examined PAP effects on strength/power activities, whereas the effects on endurance sports are understudied. The aim of this study was to characterize PAP conditioning stimulus effects on a subsequent 5x1 km running trial. A randomized, within subjects, repeated measures study utilized 12 male, endurance-trained athletes, who performed a full warm-up, conditioning exercise intervention (4x5 repetition maximum band-resisted squat jumps) or a control condition prior to a 5x1 km time trial run. Tests were conducted immediately prior to the intervention, after each kilometer, immediately following the 5x1 km run, and at seven and ten minutes post 5 km run. Measures included the interpolated twitch technique (ITT), evoked contractile properties, maximum voluntary isometric contractions (MVIC) plantar flexor force, drop jump, rating of perceived exertion, and heart rate. The PAP stimulus reduced the time to complete the run (3.6%; p = 0.07, d = 0.51), and decreased the time to complete kilometer one (8%; d = 1.08, p = 0.014). Jump height (p = 0.02; 9.2%) and reactive strength index (p = 0.035; 16%) increased with PAP. F100 (force produced in the first 100ms of the MVIC) and MVIC force with PAP increased at kilometers 3 (p = 0.04, d =0.84), 4 (p = 0.034, d = 0.29), and 7min post-run (p = 0.03, d = 0.60). Voluntary activation (ITT) increased at 7min post-run (p = 0.04, d = 0.59) with PAP, yet decreased at 7min post-run in the control condition (p = 0.03, d = 0.36). A prior band-resisted squat protocol decreased running time and improved neuromuscular properties in endurance athletes running 5x1 km.

Published

2019

57. Advanced Continuous Flow Platform for On-Demand Pharmaceutical Manufacturing.

Author

Zhang P, Weeranoppanant N, Thomas DA, Tahara K, Stelzer T, Russell MG, O'Mahony M, Myerson AS, Lin H, Kelly LP, Jensen KF, Jamison TF, Dai C, Cui Y, Briggs N, Beingessner RL, and Adamo A

Subjects

Automation, Ciprofloxacin chemical synthesis, Ciprofloxacin isolation & purification, Neostigmine chemical synthesis, Neostigmine isolation & purification, Nicardipine chemical synthesis, Nicardipine isolation & purification, Pharmaceutical Preparations isolation & purification, Triazoles chemical synthesis, Triazoles isolation & purification, Pharmaceutical Preparations chemical synthesis

Abstract

As a demonstration of an alternative to the challenges faced with batch pharmaceutical manufacturing including the large production footprint and lengthy time-scale, we previously reported a refrigerator-sized continuous flow system for the on-demand production of essential medicines. Building on this technology, herein we report a second-generation, reconfigurable and 25 % smaller (by volume) continuous flow pharmaceutical manufacturing platform featuring advances in reaction and purification equipment. Consisting of two compact [0.7 (L)×0.5 (D)×1.3 m (H)] stand-alone units for synthesis and purification/formulation processes, the capabilities of this automated system are demonstrated with the synthesis of nicardipine hydrochloride and the production of concentrated liquid doses of ciprofloxacin hydrochloride, neostigmine methylsulfate and rufinamide that meet US Pharmacopeia standards., (© 2018 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2018