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Cell Culture Engineering (Hardcover, 2006 ed.): Wei-Shu Hu Cell Culture Engineering (Hardcover, 2006 ed.)
Wei-Shu Hu
R8,138 Discovery Miles 81 380 Ships in 12 - 17 working days

Since the introduction of recombinant human growth hormone and insulin a quarter century ago, protein therapeutics has greatly broadened the ho- zon of health care. Many patients suffering with life-threatening diseases or chronic dysfunctions, which were medically untreatable not long ago, can attest to the wonder these drugs have achieved. Although the ?rst generation of p- tein therapeutics was produced in recombinant Escherichia coli, most recent products use mammalian cells as production hosts. Not long after the ?rst p- duction of recombinant proteins in E. coli, it was realized that the complex tasks of most post-translational modi?cations on proteins could only be ef?ciently carried out in mammalian cells. In the 1990s, we witnessed a rapid expansion of mammalian-cell-derived protein therapeutics, chie?y antibodies. In fact, it has been nearly a decade since the market value of mammalian-cell-derived protein therapeutics surpassed that of those produced from E. coli. A common characteristic of recent antibody products is the relatively large dose required for effective therapy, demanding larger quantities for the treatment of a given disease. This, coupled with the broadening repertoire of protein drugs, has rapidly expanded the quantity needed for clinical applications. The increasing demand for protein therapeutics has not been met exclusively by construction of new manufacturing plants and increasing total volume capacity. More - portantly the productivity of cell culture processes has been driven upward by an order of magnitude in the past decade.

Energy-Efficient High Performance Computing - Measurement and Tuning (Paperback, 2013 ed.): James H. Laros III, Kevin Pedretti,... Energy-Efficient High Performance Computing - Measurement and Tuning (Paperback, 2013 ed.)
James H. Laros III, Kevin Pedretti, Suzanne M. Kelly, Wei Shu, Kurt Ferreira, …
R1,408 Discovery Miles 14 080 Ships in 10 - 15 working days

In this work, the unique power measurement capabilities of the Cray XT architecture were exploited to gain an understanding of power and energy use, and the effects of tuning both CPU and network bandwidth. Modifications were made to deterministically halt cores when idle. Additionally, capabilities were added to alter operating P-state. At the application level, an understanding of the power requirements of a range of important DOE/NNSA production scientific computing applications running at large scale is gained by simultaneously collecting current and voltage measurements on the hosting nodes. The effects of both CPU and network bandwidth tuning are examined, and energy savings opportunities without impact on run-time performance are demonstrated. This research suggests that next-generation large-scale platforms should not only approach CPU frequency scaling differently, but could also benefit from the capability to tune other platform components to achieve more energy-efficient performance.

Cell Culture Engineering (Paperback, Softcover reprint of hardcover 1st ed. 2006): Wei-Shu Hu Cell Culture Engineering (Paperback, Softcover reprint of hardcover 1st ed. 2006)
Wei-Shu Hu
R8,033 Discovery Miles 80 330 Ships in 10 - 15 working days

Since the introduction of recombinant human growth hormone and insulin a quarter century ago, protein therapeutics has greatly broadened the ho- zon of health care. Many patients suffering with life-threatening diseases or chronic dysfunctions, which were medically untreatable not long ago, can attest to the wonder these drugs have achieved. Although the ?rst generation of p- tein therapeutics was produced in recombinant Escherichia coli, most recent products use mammalian cells as production hosts. Not long after the ?rst p- duction of recombinant proteins in E. coli, it was realized that the complex tasks of most post-translational modi?cations on proteins could only be ef?ciently carried out in mammalian cells. In the 1990s, we witnessed a rapid expansion of mammalian-cell-derived protein therapeutics, chie?y antibodies. In fact, it has been nearly a decade since the market value of mammalian-cell-derived protein therapeutics surpassed that of those produced from E. coli. A common characteristic of recent antibody products is the relatively large dose required for effective therapy, demanding larger quantities for the treatment of a given disease. This, coupled with the broadening repertoire of protein drugs, has rapidly expanded the quantity needed for clinical applications. The increasing demand for protein therapeutics has not been met exclusively by construction of new manufacturing plants and increasing total volume capacity. More - portantly the productivity of cell culture processes has been driven upward by an order of magnitude in the past decade.

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