Abstract

The circulatory system is one of the first systems that develops during embryogenesis. Angiogenesis describes the formation of blood vessels as a part of the circulatory system and is essential for organ growth in embryogenesis as well as repair in adulthood. A dysregulation of vessel growth contributes to the pathogenesis of many disorders. Thus, an imbalance between pro- and antiangiogenic factors could be observed in infantile hemangioma (IH). IH is the most common benign tumor during infancy, which appears during the first month of life. These vascular tumors are characterized by rapid proliferation and subsequently slower involution. Most IHs regress spontaneously, but in some cases they cause disfigurement and systemic complications, which requires immediate treatment. Recently, a therapeutic effect of propranolol on IH has been demonstrated. Hence, this non-selective β-blocker became the first-line therapy for IH. Over the last years, our understanding of the underlying mechanisms of IH has been improved and possible mechanisms of action of propranolol in IH have postulated. Previous studies revealed that gap junction proteins, the connexins (Cx), might also play a role in the pathogenesis of IH. Therefore, affecting gap junctional intercellular communication is suggested as a novel therapeutic target of propranolol in IH. In this review we summarize the current knowledge of the molecular processes, leading to IH and provide new insights of how Cxs might be involved in the development of these vascular tumors.

Highlights

  • The circulatory system is one of the first systems that develops during embryogenesis

  • In this review we summarize the current knowledge of the molecular processes, leading to infantile hemangioma (IH) and provide new insights of how Cxs might be involved in the development of these vascular tumors

  • In this review we summarize the current knowledge of the pathogenesis of IHs and suggest a role of Cxs in the development of these vascular tumors

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Summary

Introduction

The circulatory system is one of the first systems that develops during embryogenesis. VEGF accelerates tumor growth via different mechanisms, comprising stimulation of proliferation as well as migration, increased vascular permeability, and inhibition of apoptosis (Harris et al, 2002).

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