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The purpose of Ribozyme Protocols is to provide a helpful
compilation of protocols that will be of use- DEGREESnot only to
those with some experience of ribozymes- DEGREESbut also to those
wishing to use ribozymes for the first time. Although it is usually
impossible to cover every aspect of a scientific field, I believe
this book approaches that ideal and should help all readers perform
meaningful experiments using ribozymes. To design ribozymes, one
must consider whether the target site will be accessible; this task
can be facilitated by using computer programs that pre dict the
folding of the target RNA. Such programs are detailed in Chapters 2
and 3. If the chosen target is an RNA virus that can mutate
rapidly, it makes sense to consider those parts of the genome that
are least likely to change during viral replication. An example of
how this can be done is described in Chapter 4. Although computer
analysis may be a useful starting point to select tar get sites,
there seems, at the moment, to be no guarantee that any particular
chosen site will be efficiently cleaved. Some workers have
deliberately bypassed this problem by using libraries of ribozyme
sequences and by select ing those that actually hybridize to and/or
cleave the target; these methods are described in Chapters 5
The purpose of Ribozyme Protocols is to provide a helpful
compilation of protocols that will be of use-^not only to those
with some experience of ribozymes-^but also to those wishing to use
ribozymes for the first time. Although it is usually impossible to
cover every aspect of a scientific field, I believe this book
approaches that ideal and should help all readers perform
meaningful experiments using ribozymes. To design ribozymes, one
must consider whether the target site will be accessible; this task
can be facilitated by using computer programs that pre dict the
folding of the target RNA. Such programs are detailed in Chapters 2
and 3. If the chosen target is an RNA virus that can mutate
rapidly, it makes sense to consider those parts of the genome that
are least likely to change during viral replication. An example of
how this can be done is described in Chapter 4. Although computer
analysis may be a useful starting point to select tar get sites,
there seems, at the moment, to be no guarantee that any particular
chosen site will be efficiently cleaved. Some workers have
deliberately bypassed this problem by using libraries of ribozyme
sequences and by select ing those that actually hybridize to and/or
cleave the target; these methods are described in Chapters 5 and 6.
This scarce antiquarian book is a selection from Kessinger
Publishing's Legacy Reprint Series. Due to its age, it may contain
imperfections such as marks, notations, marginalia and flawed
pages. Because we believe this work is culturally important, we
have made it available as part of our commitment to protecting,
preserving, and promoting the world's literature. Kessinger
Publishing is the place to find hundreds of thousands of rare and
hard-to-find books with something of interest for everyone!
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