Abstract
Survivin, an inhibitor of apoptosis protein, is highly expressed in most cancers and associated with chemotherapy resistance, increased tumor recurrence, and shorter patient survival, making antisurvivin therapy an attractive cancer treatment strategy. However, growing evidence indicates that survivin is expressed in normal adult cells, particularly primitive hematopoietic cells, T lymphocytes, polymorphonuclear neutrophils, and vascular endothelial cells, and may regulate their proliferation or survival. In preclinical animal models, targeted antisurvivin therapies show efficacy without overt toxicity. However, consequences of prolonged survivin disruption in normal cells, particularly those associated with continuous renewal, have not been clearly determined. Understanding the role of survivin in normal versus malignant cells will be important in identifying strategies that maximally disrupt survivin in cancer cells with minimal effect on normal tissues. In this review, we summarize the prognostic relevance of survivin in cancer that justifies the pursuit of antisurvivin therapies and discuss differences in survivin expression between normal and cancer cells. We subsequently review expression of survivin in normal adult tissues and evaluate preclinical antisurvivin therapies reported to date in light of emerging roles for survivin in normal physiology, particularly hematopoiesis, angiogenesis, and immune function.
Highlights
The inhibitor of apoptosis protein survivin regulates apoptosis and cell cycle
Recent studies have defined a role for survivin in regulating function in normal adult cells, vascular endothelial cells [16, 25], polymorphonuclear cells [26], T cells [9, 27], erythroid cells [28], and hematopoietic progenitor cells [10, 11, 28, 29], suggesting that survivin disruption could have adverse consequences on these cells
This study indicates that growth factor – mediated expression of survivin is required to block apoptosis in terminally differentiated neutrophils
Summary
The inhibitor of apoptosis protein survivin regulates apoptosis and cell cycle. Survivin expression has been. Expression and evidence of potential function for survivin in normal tissues is accumulating, suggesting that survivin expression is not cancer specific. Recent studies have defined a role for survivin in regulating function in normal adult cells, vascular endothelial cells [16, 25], polymorphonuclear cells [26], T cells [9, 27], erythroid cells [28], and hematopoietic progenitor cells [10, 11, 28, 29], suggesting that survivin disruption could have adverse consequences on these cells. We will summarize the expression and prognostic value of survivin in cancers and its expression and function in normal adult tissues. Understanding the expression, function, and regulation of survivin in normal versus cancer cells will be critical to the design of optimal strategies to selectively eradicate cancer cells without causing adverse effects in normal tissues.
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