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Current
Pharmaceutical Design
ISSN: 1381-6128
Current Pharmaceutical Design
Volume 14, Number 2, 2008
Contents
Mechanisms of Cell Death: Life Evolution
Executive Editor: M. de Eguileor
Editorial Pp.96
Autophagy and Cell Death in Caenorhabditis elegans
Pp. 97-115
C. Samara and N. Tavernarakis
[Abstract]
Autophagy in Invertebrates: Insights Into Development,
Regeneration and Body Remodeling Pp. 116-125
G. Tettamanti, E. Saló, C. Gonzáles-Estévez,
D.A. Felix, A. Grimaldi and M. de Eguileor
[Abstract]
Cell Death in the IPLB-LdFB Insect Cell Line: Facts
and Implications Pp. 126-130
D. Malagoli
[Abstract]
Mechanisms and Immunological Roles of Apoptosis in
Molluscs Pp. 131-137
K. Terahara and K.G. Takahashi
[Abstract]
A Tale of Death and Life: Natural Apoptosis in the
Colonial Ascidian Botryllus schlosseri (Urochordata,
Ascidiacea) Pp. 138-147
L. Ballarin, P. Burighel and F. Cima
[Abstract]
Fish and Apoptosis: Molecules and Pathways Pp.
148-169
N.M.S. dos Santos, A. do Vale, M.I.R. Reis and M.T. Silva
[Abstract]
Fish and Apoptosis: Studies in Disease and Pharmaceutical
Design Pp. 170-183
M.T. Silva, A. do Vale and N.M.S. dos Santos
[Abstract]
Cell Death in Mammalian Development Pp. 184-196
C. Penaloza, S. Orlanski, Y. Ye, T. Entezari-Zaher, M.
Javdan and Z. Zakeri
[Abstract]
Abstracts
[Back to top]
Editorial: Mechanisms of Cell Death:
Life Evolution
Extensive studies have been devoted to mechanisms leading
to the activation of cell death. Three major types of cell
death are distinguished based on different criteria: apoptosis,
oncosis and autophagic cell death. All these processes are
well conserved in life evolution as highlighted in the reviews
here gathered.
Samara and Tavernarakis review the current understanding of
cell death pathways in Caenorhabditis elegans, focusing
on autophagy, the main cellular process for bulk protein and
organelle recycling, in nematode cell death. These studies
reveal that autophagic mechanisms have a prominent role in
both apoptosis and necrosis.
Tettamanti et al. summarize recent findings on the
role of autophagy in two different invertebrate taxa, Platyhelminthes
and Insects, focusing attention on two complex events occurring
in those systems, namely planarian regeneration and insect
metamorphosis. Both represent good models in which to investigate
the process of autophagy and its relationship with other programmed
cell death mechanisms.
Malagoli highlights the findings on stress-induced cell death
in a new in vitro invertebrate model, i.e. the IPLB-LdFB
insect cell line derived from the larval fat body of the lepidopteron
Lymantria dispar. Apoptotic, oncotic and autophagic
cell death have been described in these cells as a consequence
of oxidative stress or ATP deprivation, and similarities between
IPLB-LdFB and mammalian apoptotic pathways have been demonstrated.
Terahara and Takahashi focus on immunological roles and molecular
mechanisms of apoptosis related to functions of hemocytes
in molluscan species living in an environment that changes
incessantly according to microorganisms, industrial pollutants,
temperature, and salinity. Such environmental factors might
directly or indirectly induce apoptosis in molluscan cells.
Ballarin et al. reported in the the ascidian Botryllus
schlosseri natural apoptosis can be studied in different
phases of colony life. From these results B. schlosseri
is proposed as a new invertebrate species alternative to Drosophila
and Caenorhabditis for the study of apoptosis.
Dos Santos et al. in their article review structural
and functional data on the most important apoptosis-related
molecules, namely death-receptor, Bcl-2 and caspase families,
and mechanisms. The data point to the existence in fish of
apoptotic pathways equivalent to those of mammals.
Silva et al. advance the knowledge about fish on
the role of apoptosis in viral infections and of apoptosis
and necrosis in bacterial infections. The use of fish for
research on apoptosis-related issues relevant for human physiology
and pathology and for the design of apoptosis-modulating drugs
will continue to increase.
Penaloza et al. discuss the types and distributions
of cell death in developing mammalian embryos as well as the
gene products that may regulate the process. Several types
of cell death, as identified by their morphological and biochemical
features, can be seen in embryos, tissues associated with
pregnancy, and in adult organisms. Cell deaths help sculpt
the embryo from the grossest to the finest details of its
development. Developmental abnormalities can be traced to
aberrant patterns of cell death.
References
[1] Samara C, Tavernarakis N. Autophagy and cell death in
Caenorhabditis elegans. Curr Pham Des 2008; 14(2):
97-115.
[2] Tettamanti G, Saló E, Gonzáles-Estévez
C, Felix DA, Grimaldi A, de Eguileor M. Autophagy in invertebrates:
insights into development, regeneration and body remodeling.
Curr Pham Des 2008; 14(2): 116-125.
[3] Malagoli D. Cell death in the IPLB-LdFB insect cell line:
Facts and implications. Curr Pham Des 2008; 14(2): 126-130.
[4] Terahara K, Takahashi KG. Mechanisms and immunological
roles of apoptosis in molluscs. Curr Pham Des 2008; 14(2):
131-137.
[5] Ballarin L, Burighel P, Cima F. A tale of death and life:
Natural apoptosis in the colonial ascidian Botryllus schlosseri
(Urochordata, Ascidiacea). Curr Pham Des 2008; 14(2): 138-147.
[6] dos Santos NMS, do Vale A, Reis MIR, Silva MT. Fish and
apoptosis: Molecules and pathways. Curr Pham Des 2008; 14(2):
148-169.
[7] Silva MT, do Vale A, dos Santos NMS. Fish and apoptosis:
Studies in disease and pharmaceutical design. Curr Pham Des
2008; 14(2): 170-183.
[8] Penaloza C, Orlanski S, Ye Y, Entezari-Zaher T, Javdan
M, Zakeri Z. Cell death in mammalian development. Curr Pham
Des 2008; 14(2): 184-196.
Magda de Eguileor
Department of Structural and Functional Biology
University of Insubria
Via J.H. Dunant 3
21100 Varese
Italy
E-mail: magda.deeguileor@uninsubria.it
[Back to top]
Autophagy and Cell Death in Caenorhabditis elegans
C. Samara and N. Tavernarakis
Cell death is a major component of developmental programs.
Controlled killing of specific cells at appropriate time points
is required for normal growth and shaping of organisms. However,
cellular demolition can also result in a variety of pathologies
that are frequently fatal, when implemented inappropriately.
Delineation of cell death mechanisms has been greatly facilitated
by the use of simple model organisms such as the nematode
worm Caenorhabditis elegans. Research in C. elegans
has proven instrumental for the elucidation of the molecular
mechanisms underlying both apoptotic and necrotic cell death.
Here, we introduce the C. elegans model and review
the current understanding of cell death pathways in this organism.
We further focus on recent studies implicating autophagy,
the main cellular process for bulk protein and organelle recycling,
in nematode cell death. These studies reveal that autophagic
mechanisms have a prominent role in both apoptosis and necrosis.
We survey the relevant findings in C. elegans and
also consider the contribution of autophagy in cell death
in other experimental systems. Comparative analysis suggests
that the involvement of autophagy in cell death is evolutionary
conserved in metazoans. Thus, interfering with the autophagic
process may facilitate therapeutic intervention in human pathologies
where aberrant cell death is a contributing factor.
[Back to top]
Autophagy in Invertebrates: Insights Into Development, Regeneration
and Body Remodeling
G. Tettamanti, E. Saló, C. Gonzáles-Estévez,
D.A. Felix, A. Grimaldi and M. de Eguileor
Autophagy is a process in which eukaryotic cells sequester
and degrade cytoplasm and organelles via the lysosomal
pathway. This process allows turnover of intracellular organelles,
participates in the maintenance of cellular homeostasis and
prevents accumulation of defective cellular structures.
Increased autophagy is normally induced by environmental cues
such as starvation and hormones, while excessive levels of
autophagy can lead to autophagic programmed cell death (PCD),
with features that differ from those of the apoptotic PCD
process.
Since autophagic PCD plays a key role in development, morphogenesis
and regeneration in several animal taxa, identification of
evolutionarily conserved components of the autophagic machinery
is a basic starting point in order to unravel the role of
autophagy under both physiological and pathological conditions.
Here we summarize recent findings on the role of autophagy
in two different invertebrate taxa, Platyhelminthes and Insects,
focusing attention on two complex events occurring in those
systems, namely planarian regeneration and insect metamorphosis.
Both represent good models in which to investigate the process
of autophagy and its relationship with other PCD mechanisms.
[Back to top]
Cell Death in the IPLB-LdFB Insect Cell Line: Facts and Implications
D. Malagoli
The present review summarizes findings on stress-induced
cell death in the IPLB-LdFB insect cell line derived from
the larval fat body of the lepidopteron Lymantria dispar.
Apoptotic, oncotic and autophagic cell death have been described
in these cells as a consequence of oxidative stress or ATP
deprivation, and similarities between IPLB-LdFB and mammalian
apoptotic pathways have been highlighted. Furthermore, starting
from observations in the IPLB-LdFB cells, a link has been
surmised between relevance of autophagic cell death and developmental
processes in the metazoan taxa.
[Back to top]
Mechanisms and Immunological Roles of Apoptosis in Molluscs
K. Terahara and K.G. Takahashi
Molluscan defense mechanisms are regulated to innate immunity,
which is largely dependent on cellular components such as
hemocytes possessing phagocytic and bactericidal activities.
Among immune responses, apoptosis is an indispensable process
because it enables the adequate clearance of damaged, senescent
and infected cells without inflammation. Available information
related to the molecular mechanisms of apoptosis has been
accumulated for many molluscan species during the last decade.
Almost all molluscan species live in an environment that changes
incessantly according to microorganisms, industrial pollutants,
temperature, and salinity. Such environmental factors might
directly or indirectly induce apoptosis in molluscan cells.
One type of apoptotic agent, reactive oxygen intermediates
(ROIs), which are produced by a stress signal or phagocytosis,
triggers apoptotic cell death in molluscan hemocytes. Dysfunction
of ROI-mediated hemocytic apoptosis putatively causes disease
morbidity and/or mortality when molluscan organisms are infected
by pathogens. Furthermore, integrins have attracted attention
for their unique functions because integrins regulate the
phagocytic ability of molluscan hemocytes and induce hemocytic
apoptosis. That process might be the result of ROI-generation.
In this review, we summarize the roles and molecular mechanisms
of apoptosis related to immunological functions of molluscan
hemocytes.
[Back to top]
A Tale of Death and Life: Natural Apoptosis in the Colonial
Ascidian Botryllus schlosseri (Urochordata, Ascidiacea)
L. Ballarin, P. Burighel and F. Cima
The colonial ascidian Botryllus schlosseri forms
new zooids by blastogenesis, through the formation of palleal
buds which progressively grow and mature until adults are
formed. At a temperature of 19°C, adult zooids remain
active for about one week; then they contract, close their
siphons and are gradually resorbed, being replaced by buds
which reach functional maturity, open their siphons and begin
their filtering activity as adult zooids. This recurrent generation
change, known as take-over, is characterised by the occurrence
of diffuse programmed cell death by apoptosis. Immediately
before the take-over, an increase in the expression of molecules
recognised by anti-Bax antibodies and a parallel decrease
in the expression of molecules immunopositive to anti-Bcl-2
antibodies were observed in zooid tissues, suggesting a mitochondrion-dependent
apoptotic pathway. During the take-over, circulating phagocytes
infiltrate the zooid tissues and engulf apoptotic cells; in
addition, the frequency of haemocytes showing nuclear condensation
and annexin-V labelling significantly increases. Previous
experiments showed the involvement of phosphatidylserine and
CD36 in the recognition of effete cell. The resorption of
old zooids is closely related to the rejuvenation of the colony
occurring at the take-over. The death of adult zooids puts
a quantity of material at the colony disposal. This material
is represented by senescent cells, which, once ingested and
digested by phagocytes, can be recycled and used to sustain
the burden of blastogenesis: this involves a cross-talk between
old tissues, phagocytes and developing buds. Therefore, B.
schlosseri can be considered a new and promising model
organism for the study of natural apoptosis.
[Back to top]
Fish and Apoptosis: Molecules and Pathways
N.M.S. dos Santos, A. do Vale, M.I.R. Reis and M.T. Silva
Apoptosis is a genetically controlled and evolutionarily conserved
form of active cell death, albeit with an increase in complexity
with continuing development. A high conservation at the functional
and molecular level has been described between the players
of the apoptotic machinery in invertebrates (Caenorhabditis
elegans and Drosophila) and mammals. However, fish represent
an excellent and advantageous model for the study of vertebrate
development and disease, bridging the gap between the C.
elegans/Drosophila and mouse/human models. Moreover,
contrary to C. elegans and Drosophila, fish can be
used for studying the development and function of vertebrate-specific
organs and have a fully developed immune system similar to
that of mammals. Last but not less important, both the environment
and human health will obviously gain by using the knowledge
generated through the use of fish models, for developing better
prophylactic and therapeutic measures with impact on the aquaculture
industry. In the present article, structural and functional
data on the most important apoptosis related molecules, namely
death-receptor, Bcl-2 and caspase families, and mechanisms
are reviewed. The data point to the existence in fish of apoptotic
pathways equivalent to those of mammals, making fish useful
animal models for studying apoptosis, which may have great
applicability for the advance of the knowledge on the role
of apoptotic cell death in human apoptosis-related disorders
as well as in pharmaceutical design
[Back to top]
Fish and Apoptosis: Studies in Disease and Pharmaceutical
Design
M.T. Silva, A. do Vale and N.M.S. dos Santos
The relevance of fish research has been rising due to
the expansion of aquaculture and to the increasing use of
fish as replace-ments for mammals in the study of human physiological
and pathological issues. Fish have much smaller genomes compared
to mammals, and zebrafish, fugu, medaka and spotted green
puffer fish have the sequence of their genomes completed or
near completion. Fish have several of the virtues of Drosophila
melanogaster and Caenorhabditis elegans for
apoptosis research, but offer additional advantages because
they are vertebrates and have a developed immune system and
apoptotic pathways similar to those of mammals. Many phenotypes
in the zebrafish resemble human diseases and this fish has
been increasingly used in pharmaceutical design of apoptosis
modulating drugs. The roles of microRNAs, bcl-2, p53, insulin-like
growth factor-binding protein-3, and cellular apoptosis susceptibility
(CAS) and c-Myc genes (involved in the interaction apoptosis/cancer),
and Aβ
peptides, presenilin enhancer 2, cyclin-dependent kinase 5
and tau (factors with relevant roles in apoptosis-associated
human neurodegenerative disorders), have also been successfully
investigated in fish models. Results of research with fish
that have advanced the knowledge on the participation of apoptosis
in viral infections and of apoptosis and secondary necrosis
in bacterial infections are also reviewed. It is expectable
that the use of fish for research on apoptosis-related issues
relevant for human physiology and pathology and for the design
of apoptosis-modulating drugs will continue to increase.
[Back to top]
Cell Death in Mammalian Development
C. Penaloza, S. Orlanski, Y. Ye, T. Entezari-Zaher, M.
Javdan and Z. Zakeri
During embryogenesis there is an exquisite orchestration
of cellular division, movement, differentiation, and death.
Cell death is one of the most important aspects of organization
of the developing embryo, as alteration in timing, level,
or pattern of cell death can lead to developmental anomalies.
Cell death shapes the embryo and defines the eventual functions
of the organs. Cells die using different paths; understanding
which path a dying cell takes helps us define the signals
that regulate the fate of the cell. Our understanding of cell
death in development stems from a number of observations indicating
genetic regulation of the death process. With today’s
increased knowledge of the pathways of cell death and the
identification of the genes whose products regulate the pathways
we know that, although elimination of some of these gene products
has no developmental phenotype, alteration of several others
has profound effects. In this review we discuss the types
and distributions of cell death seen in developing mammalian
embryos as well as the gene products that may regulate the
process.
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