4.8 Article

The Epstein-Barr virus noncoding RNA EBER2 transactivates the UCHL1 deubiquitinase to accelerate cell growth

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.2115508118

Keywords

Epstein-Barr virus; B cell lymphomas; UCHL1; noncoding RNA EBER2

Funding

  1. DKFZ [F100]
  2. Institut National de la Sante et de la Recherche Medicale [U1074]
  3. Ministry of Science and Technology (MOST) of Taiwan [MOST 109-2636-B-010-007]
  4. MOST [109-2636-B-010-007]

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The viral noncoding RNA EBER2 accelerates B cell growth by potentiating expression of the UCHL1 deubiquitinase, even in Burkitt's lymphoma cells that do not express the virus's known oncogenes. This study identifies a direct cellular target of a viral noncoding RNA that is likely crucial for EBV's oncogenic properties.
The Epstein-Barr virus (EBV) transforms resting B cells and is involved in the development of B cell lymphomas. We report here that the viral noncoding RNA EBER2 accelerates B cell growth by potentiating expression of the UCHL1 deubiquitinase that itself increased expression of the Aurora kinases and of cyclin B1. Importantly, this effect was also visible in Burkitt's lymphoma cells that express none of the virus's known oncogenes. Mechanistically, EBER2 bound the UCHL1 messenger RNA (mRNA), thereby bringing a protein complex that includes PU.1, a UCHL1 transactivator, to the vicinity of its promoter. Although the EBV oncogene LMP1 has been suggested to induce UCHL1, we show here that EBER2 plays a much more important role to reach significant levels of the deubiquitinase in infected cells. However, some viruses that carried a polymorphic LMP1 had an increased ability to achieve full UCHL1 expression. This work identifies a direct cellular target of a viral noncoding RNA that is likely to be central to EBV's oncogenic properties.

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