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Review Article

The role of microRNAs in the pathogenesis of HIV-related lymphomas

, , , , , , , & show all
Pages 232-241 | Received 26 Nov 2014, Accepted 12 Mar 2015, Published online: 28 Jul 2015
 

Abstract

The incidence of HIV-related lymphomas (HRLs) is increased by 60–100 times in patients with HIV. When compared to the general population, patients with HRLs often present with extranodal lymphoid proliferation, most frequently of the gastrointestinal tract, central nervous system, liver and bone marrow. MicroRNAs (miRs) are non-coding double-stranded RNA molecules of 18–25 nucleotides that regulate post-translational gene expression by inhibiting translation or promoting degradation of messenger RNA complementary sequences. Before their discovery, tumorigenesis was thought to have been caused by the alteration of protein-coding oncogenes and tumor-suppressor genes, but once identified in B-cell chronic lymphocytic leukemia, miRs function as either oncogenes or tumor-suppressor genes was confirmed in different types of malignancies. Since miRs are clearly involved in tumorigenesis in many cancers, their role in HRLs is now receiving attention. A few studies have been conducted thus far in some HRLs on the involvement of miR in the pathogenesis of lymphoid malignancies. Since B-cell lymphomas arise from various stages of B-cell development in both HIV-infected and HIV-naïve patients, investigators have tried to determine the different miR signatures in B-cell development. As classic immunohistochemistry staining is sometimes not enough for the differential diagnosis of HRLs, in the present review, we have described the potential use of miRs in the prognosis and diagnosis of these diseases.

Declaration of interest

The current paper is supported by an international grant, Romania–European Economical Space (Norway), which was awarded to Andrei Cucuianu and Ciprian Tomuleasa (contract 1/16.01.2014). This paper was published under the frame of European Social Fund, Human Resources Development Operational Programme 2007–2013, Project number POSDRU 159/1.5/138776. All authors have read and approved the final version of the manuscript. No potential conflicts of interest are declared.

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