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Experts from around the world review the current field of the
immunobiology of heat shock proteins, and provide a comprehensive
account of how these molecules are spearheading efforts in the
understanding of various pathways of the immune system. This
one-stop resource contains numerous images to both help illustrate
the research on heat shock proteins, and better clarify the field
for the non-expert. Heat shock proteins (HSPs) were discovered in
1962 and were quickly recognized for their role in protecting cells
from stress. Twenty years later, the immunogenicity of a select few
HSPs was described, and for the past 30 years, these findings have
been applied to numerous branches of immunology, including tumor
immunology and immunosurveillance, immunotherapy, etiology of
autoimmunity, immunotherapy of infectious diseases, and expression
of innate receptors. While HSPs can be used to manipulate immune
responses by exogenous administration, they appear to be involved
in initiation of de novo immune responses to cancer and likely in
the maintenance of immune homeostasis.
Experts from around the world review the current field of the
immunobiology of heat shock proteins, and provide a comprehensive
account of how these molecules are spearheading efforts in the
understanding of various pathways of the immune system. This
one-stop resource contains numerous images to both help illustrate
the research on heat shock proteins, and better clarify the field
for the non-expert. Heat shock proteins (HSPs) were discovered in
1962 and were quickly recognized for their role in protecting cells
from stress. Twenty years later, the immunogenicity of a select few
HSPs was described, and for the past 30 years, these findings have
been applied to numerous branches of immunology, including tumor
immunology and immunosurveillance, immunotherapy, etiology of
autoimmunity, immunotherapy of infectious diseases, and expression
of innate receptors. While HSPs can be used to manipulate immune
responses by exogenous administration, they appear to be involved
in initiation of de novo immune responses to cancer and likely in
the maintenance of immune homeostasis.
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