Current
Pharmaceutical Biotechnology
ISSN: 1389-2010
Current Pharmaceutical Biotechnology
Volume 8, Number 4, August 2007
Contents
Medicinal Plant Biotechnology
Guest Editors: K. Saito and M. Yamazaki
Editorial Pp. 195
Camptothecin: Therapeutic Potential and Biotechnology
Pp. 196-202
S. Sirikantaramas, T. Asano, H. Sudo, M. Yamazaki and
K. Saito
[Abstract]
Tropane and Nicotine Alkaloid Biosynthesis-Novel Approaches
Towards Biotechnological Production of Plant-Derived Pharmaceuticals
Pp. 203-210
K.-M. Oksman-Caldentey
[Abstract]
Metabolic Engineering in Isoquinoline Alkaloid Biosynthesis
Pp. 211-218
F. Sato, T. Inui and T. Takemura
[Abstract]
Advancements in the Understanding of Paclitaxel Metabolism
in Tissue Culture Pp. 219-236
K. Vongpaseuth and S.C. Roberts
[Abstract]
Recent Advances in Cannabis sativa Research:
Biosynthetic Studies and Its Potential in Biotechnology
Pp. 237-243
S. Sirikantaramas, F. Taura, S. Morimoto and Y. Shoyama
[Abstract]
Accumulation and Membrane Transport of Plant Alkaloids
Pp. 244-252
N. Shitan and K. Yazaki
[Abstract]
Abstracts
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Editorial
Since the ancient times plants have been rich sources
of medicines. This is still true even in the modernized Societies.
New natural compounds potentially leading to innovative drugs
are being discovered from plants. We are often astonished
by how much man enjoys the benefits of the huge chemical diversity
of plants not only for providing medicines but also pesticides,
flavors, dyes and other industrial materials. More recently
plant biotechnology, including cell culture and genetic manipulation,
offers new possibilities for the development of more effective
pharmaceuticals and feasible production of drugs from plants.
This Special Issue aims to review the state-of-the-art for
medicinal plant biotechnology. All six articles deal with
plant-derived compounds which are clinically used nowadays.
These chapters are contributed by the leading scientists from
throughout the world. They describe the current status of
biosynthesis and accumulation of pharmaceutical compounds
in plants and plant cell cultures, gene identification for
the production of these compounds, and future prospects of
medicinal plant biotechnology.
We hope this Special Issue will carry the torch for the research
on medicinal plants in the future, and we look forward to
breakthrough innovations in drug developments through modern
plant biotechnology.
Kazuki Saito
Mami Yamazaki
[Back to top]
Camptothecin: Therapeutic Potential and Biotechnology
S. Sirikantaramas, T. Asano, H. Sudo, M. Yamazaki and
K. Saito
Camptothecin (CPT) and its derivatives have been received
considerable attention recently. Two semi-synthetic derivatives,
topotecan and irinotecan, are currently prescribed as anticancer
drugs. Several more are now in clinical trial. CPT is produced
in many plants belonging to unrelated orders of angiosperms.
At present, CPT supplied for pharmaceutical use is extracted
from the plants, Camptotheca acuminata and Nothapodytes
foetida. Several efforts have been made to sustain a
stable production of CPT by in vitro cell cultures of C.
acuminata, N. foetida and Ophiorrhiza pumila.
Recent report showed that plants are not the only sources
that produce CPT. CPT was reported to be produced from the
endophytic fungus isolated from the inner bark of N. foetida.
The hairy root cultures of C. acuminata
and O. pumila produce and secrete CPT into the medium
in large quantities. These reports suggest the possibility
to develop large-scale production of CPT. In addition, recent
advance in the cloning and characterization of biosynthetic
enzymes involved in CPT bio-synthetic pathway provides valuable
information for developing genetically engineered CPT-producing
plants.
[Back to top]
Tropane and Nicotine Alkaloid Biosynthesis-Novel Approaches
Towards Biotechnological Production of Plant-Derived Pharmaceuticals
K.-M. Oksman-Caldentey
Many plants belonging to the Solanaceae family have been used
as a source of pharmaceuticals for centuries because of their
active principles, tropane and nicotine alkaloids. Tropane
alkaloids, atropine, hyoscyamine and scopolamine, are among
the oldest drugs in medicine. On the other hand nicotine,
the addictive agent in tobacco, has only recently gained attention
as a backbone for novel potential alkaloids to be used for
certain neurological diseases. The biotechnological production
of alkaloids utilizing plant cells as hosts would be an attractive
option. However, to date very little success in this field
has been gained because of the lack of understanding how these
compounds are synthesized in a plant cell. Metabolic engineering
attempts have already shown that when the rate-limiting steps
of the biosynthetic pathway are completely known and the respective
genes cloned, the exact regulation towards desired medicinal
products will be possible in the near future. The new functional
genomics tools, which combine transcriptome and metabolome
data, will create a platform to better understand a whole
system and to engineer the complex plant biosynthetic pathways.
With the help of this technology, it is not only possible
to produce known plant metabolites more effectively but also
to make arrays of new compounds in plants and cell cultures.
[Back to top]
Metabolic Engineering in Isoquinoline Alkaloid Biosynthesis
F. Sato, T. Inui and T. Takemura
Higher plants produce diverse classes of metabolites. Metabolic
engineering offers tremendous potential to improve the production
and quality of these chemicals. This report summarizes the
possibility of using metabolic engineering in benzylisoquinoline
alkaloid biosynthesis. Benzylisoquinoline alkaloids, such
as morphine, sanguinarine, and berberine, are synthesized
from tyrosine via reticuline in Magnoliaceae, Ranunculaceae,
Berberidaceae, Papaveraceae, and many other species. The early
pathway from tyrosine to reticuline is common among many plant
species, whereas there is more diversity in late pathways.
This review describes several strategies to improve the yield
and quality of benzylisoquinoline alkaloids. First, the overexpression
of a rate-limiting enzyme in an early pathway to increase
the overall alkaloid yield is discussed. Second, the introduction
of a new branch into the pathway has been shown to produce
novel metabolites. Finally, the possibility of accumulating
a pathway intermediate by the knock-down of a key step is
examined. Further metabolic modification is also discussed,
since the latter two modifications may lead to the production
of novel compound(s) from an accumulated intermediate through
metabolic activation. These metabolic changes could be further
modified to increase chemical diversity through somatic variation
in cell culture. Besides this direct metabolic engineering
with isolated biosynthetic genes, the regulation of biosynthetic
activity with transcription factors and/or with reconstruction
of the entire biosynthesis will also be discussed for the
next generation of metabolite production.
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Advancements in the Understanding of Paclitaxel Metabolism
in Tissue Culture
K. Vongpaseuth and S.C. Roberts
Paclitaxel is a potent chemotherapeutic agent approved in
the treatment of a variety of cancers, and under evaluation
for the treatment of Alzheimer’s and heart disease.
Originally isolated from Taxus brevifolia, this highly
substituted ring diterpenoid belongs to a family of plant
secondary metabolites known as taxoids. Paclitaxel is currently
suppl ied through both a semi-synthetic process and plant
cell culture. Taxus spp. cell culture offers the
potential to produce large amounts of paclitaxel and related
taxoids, although variability in accumulation and low yields
represent key limitations. Thus, intense efforts have been
put forth towards understanding Taxus spp. metabolism
to increase paclitaxel accumulation in cell culture. While
elicitation and environmental optimization have provided some
success in increasing paclitaxel accumulation in vitro,
understanding metabolism of paclitaxel on the molecular level
is essential for process optimization. Utilizing direct and
indirect molecular techniques, a further understanding of
paclitaxel biosynthesis has been gained, though knowledge
into other aspects of paclitaxel global metabolism, such as
regulation, transport, and degradation is lacking. Taxus
spp. cell cultures are highly heterogeneous, displaying
significant cell-cell variability in growth and paclitaxel
accumulation. Information gathered on culture subpopulations
as well as putative transcriptional bottlenecks in paclitaxel
biosynthesis, coupled with successful transformation of Taxus
spp. will allow for the targeted metabolic engineering
of Taxus spp. or other model organisms for paclitaxel
accumulation to ensure future supply of this important pharmaceutical.
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Recent Advances in Cannabis sativa Research:
Biosynthetic Studies and Its Potential in Biotechnology
S. Sirikantaramas, F. Taura, S. Morimoto and Y. Shoyama
Cannabinoids, consiting of alkylresorcinol and monoterpene
groups, are the unique secondary metabolites that are found
only in Cannabis sativa. Tetrahydrocannabinol (THC),
cannabidiol (CBD) and cannabichromene (CBC) are well known
cannabinoids and their pharmacological properties have been
extensively studied. Recently, biosynthetic pathways of these
cannabinoids have been successfully established. Several biosynthetic
enzymes including geranylpyrophosphate:olivetolate geranyltransferase,
tetrahydrocannabinolic acid (THCA) synthase, cannabidiolic
acid (CBDA) synthase and cannabichromenic acid (CBCA) synthase
have been purified from young rapidly expanding leaves of
C. sativa. In addition, molecular cloning, characterization
and localization of THCA synthase have been recently reported.
THCA and cannabigerolic acid (CBGA), its substrate, were shown
to be apoptosis-inducing agents that might play a role in
plant defense. Transgenic tobacco hairy roots expressing THCA
synthase can produce THCA upon feeding of CBGA. These results
open the way for biotechnological production of cannabinoids
in the future.
[Back to top]
Accumulation and Membrane Transport of Plant Alkaloids
N. Shitan and K. Yazaki
Among a large number of plant secondary metabolites, alkaloids
comprise one of the most important groups due to their strong
and divergent biological activities, and some are applied
for clinical use. Alkaloids are often highly accumulated in
particular organs of medicinal plants, which are called the
‘medicinal part’, whereas it is known that some
alkaloids are translocated from source organs to such sink
organs. The movement of biosynthetic intermediates from specific
cells to other types of cells in tissue, and further detailed
movement within the organelles in a cell is also suggested.
However, little is known how alkaloids are transported across
membranes and finally accumulated in specific organelles such
as vacuole of the sink organ. To increase the productivity
of valuable alkaloids in planta, not only
biosynthetic genes of alkaloids but also genes involved in
their transport will be important. Recently, the involvement
of ABC transporters in the translocation of berberine alkaloid
from root to rhizome was reported, while H+
antiporters were also suggested as the responsible transporters
for vacuolar accumulation of the alkaloid. In this review,
we describe intra-organ, intra-tissue and intra-cellular transport
of the alkaloid via membrane transports. Furthermore,
we discuss the possibility of increasing alkaloid production
in transgenic plants by using alkaloid transporter genes.
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