Kaposi sarcoma herpesvirus–induced cellular reprogramming contributes to the lymphatic endothelial gene expression in Kaposi sarcoma

Wang, Hsei‐Wei; Trotter, Matthew; Lagos, Dimitrios; Bourboulia, Dimitra; Henderson, Stephen; Mäkinen, Ta ija; Elliman, Stephen J.; Flanagan, Adrienne M.; Alitalo, Kari; Boshoff, Chris

doi:10.1038/ng1384

Cited by 415 publications

(461 citation statements)

References 28 publications

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“…IGF-IR was detected by immunohistochemistry in tumor spindle cells (Catrina et al, 2005). Overexpression of the IR in KS tissue compared to normal skin was reported by Wang et al (2004) in a comprehensive microarray study, and we have independently shown that IR gene expression is induced in KSHV-infected primary DMVEC, AIDS-KS tissue and TIME cells. Furthermore, we show that the upregulated IR is phosphorylated and we observed increased activation of the downstream Erk pathway, but not the PI3K pathway, in KSHV-infected cells.…”

Section: Discussionsupporting

confidence: 58%

The insulin receptor is essential for virus-induced tumorigenesis of Kaposi's sarcoma

Rose

Carroll

et al. 2006

Oncogene

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Section: Discussionsupporting

confidence: 58%

The insulin receptor is essential for virus-induced tumorigenesis of Kaposi's sarcoma

Rose

Carroll

et al. 2006

Oncogene

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“…Recent gene expression profiling analyses have shown that spindle cells, which form the major cellular component of the lesions, most closely resemble lymphatic endothelium [19]. The lesions also contain a variable inflammatory and mononuclear cell infiltrate.…”

Section: Developing a Better Understanding Of Ks Pathogenesismentioning

confidence: 99%

“…The lesions also contain a variable inflammatory and mononuclear cell infiltrate. Studies published beginning in the late 1980s indicated that spindle cells derived from KS lesions could release, proliferate, and/or migrate in response to various growth factors that stimulate angiogenesis, including vascular endothelial growth factor (VEGF), basic fibroblast growth factor (bFGF), interleukins -1, -6 and -8, and platelet-derived growth factor (PDGF), and over-express receptors for multiple cytokines [19][20][21][22]. Activation of these receptors stimulates multiple pro-growth and anti-apoptotic pathways via PI3kinase/Akt/mTOR and extracellular receptor kinase (ERK) [23].…”

Section: Developing a Better Understanding Of Ks Pathogenesismentioning

confidence: 99%

AIDS-associated Kaposi's sarcoma: Is there still a role for interferon alfa?

Krown

2007

Cytokine & Growth Factor Reviews

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Interferon alfa (IFNA) was one of the first agents to be used therapeutically in AIDS-associated Kaposi's sarcoma (KS) more than 25 years ago, and induces tumor regression in a subset of patients. Although much has been learned about the clinical role of IFNα in KS treatment, little is currently known about the mechanism(s) by which IFNA causes KS regression. This is despite a growing understanding of both KS pathogenesis and relevant IFNA activities. To a large extent other agents have supplanted IFNA as treatments for KS, but there may still remain a therapeutic role for IFNA, possibly in combination with other agents targeting angiogenesis and/or HHV-8-encoded human gene homologs that encode proteins involved in cell cycle regulation and signaling. KeywordsInterferon; Kaposi's sarcoma In 1995, when I was honored as a recipient of the ISICR Milstein Award, the AIDS epidemic had recently begun its 15 th year and the human immunodeficiency virus (HIV-1) had been isolated some 12 years previously [1]. However, the virus associated with Kaposi's sarcoma (KS), the most common AIDS-associated malignancy, had been described less than a year earlier [2], its significance was still in some question and its role in KS development had not been characterized, and the active combination drug regimens with which we now treat HIV infection had not yet become widely available. Recombinant interferon alfa preparations (IFNα2a and IFNα2b), which had received approval from the U.S. Food and Drug Administration (FDA) for treatment of AIDS-associated KS in 1988, were still the only approved drugs for systemic treatment of KS (the chemotherapeutic agent, liposomal doxorubicin, would receive FDA approval later in 1995, as did liposomal daunorubicin in 1996 and paclitaxel in 1997). Now, more than a quarter century after the first published reports describing AIDS and its association with KS [3-6] and our first modestly successful attempts to treat KS with IFNα [7], this agent is used infrequently to treat KS, although it still finds use in HIV-infected individuals co-infected with hepatitis C. In this brief review, I will summarize some of the history of IFNα in the treatment of AIDS-associated KS, concentrating on examples of clinical trials in which I have personally been involved, and consider whether there remains a potentially valuable role for this agent in KS treatment.

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“…This KSHV-mediated upregulation of Prox1 leads to reprogramming of BEC to adopt LEC phenotypes by overexpressing more than 70% of lymphatic-associated genes and by downregulating many BEC-specific genes ). In contrast, expression of Prox1 is downregulated in KSHV-infected cultured LEC, which is associated with a transcriptional drift toward to BEC (Wang et al, 2004). This Prox1-mediated cell fate reprogramming in KSHV-infected cells provides an additional support to the notion that Prox1 is a master control gene specifying lymphatic endothelial cell fates Wang et al, 2004).…”

Section: Prox1mentioning

confidence: 80%

Development of the lymphatic vascular system: A mystery unravels

Hong

Shin

Detmar

2004

Developmental Dynamics

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The blood vascular and the lymphatic system play complementary roles in tissue perfusion and fluid reabsorption. Despite its critical role in mediating tissue fluid homeostasis, intestinal lipid absorption, and the immune response, the lymphatic system has not received as much attention as the blood vascular system, largely due to a lack of lymphatic-specific markers and to the dearth of knowledge about the molecular regulation of lymphatic development and function. A series of recent landmark studies now significantly has advanced our understanding of the lymphatic system. Based upon the discovery and characterization of lymphatic-specific growth factors, receptors, and transcriptional regulators, the mystery of lymphatic vascular system development begins to be unraveled. The successful isolation and cultivation of blood vascular and lymphatic endothelial cells has enabled comparative molecular and cellular analyses of these two genetically and developmentally closely related cell lineages. Moreover, studies of several genetic mouse models have set the framework for a new molecular model of embryonic lymphatic vascular development and have identified molecular pathways whose mutational inactivation leads to human diseases associated with lymphedema. Although these rapid advances already have led to development of the first lymphatic-targeted molecular therapies, there still remain many unanswered questions regarding almost every aspect of lymphatic vascular biology, making the lymphatic system a highly exciting and rewarding field of study.

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Kaposi sarcoma herpesvirus–induced cellular reprogramming contributes to the lymphatic endothelial gene expression in Kaposi sarcoma

Cited by 415 publications

References 28 publications

The insulin receptor is essential for virus-induced tumorigenesis of Kaposi's sarcoma

The insulin receptor is essential for virus-induced tumorigenesis of Kaposi's sarcoma

AIDS-associated Kaposi's sarcoma: Is there still a role for interferon alfa?

Development of the lymphatic vascular system: A mystery unravels

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