BAP1 forms a trimer with HMGB1 and HDAC1 that modulates gene × environment interaction with asbestos.


Carriers of heterozygous germline <i>BAP1</i> mutations (<i>BAP1</i><sup>+/-</sup>) are affected by the "BAP1 cancer syndrome." Although they can develop almost any cancer type, they are unusually susceptible to asbestos carcinogenesis and mesothelioma. Here we investigate why among all carcinogens, <i>BAP1</i> mutations cooperate with asbestos. Asbestos carcinogenesis and mesothelioma have been linked to a chronic inflammatory process promoted by the extracellular release of the high-mobility group box 1 protein (HMGB1). We report that <i>BAP1</i><sup>+/-</sup> cells secrete increased amounts of HMGB1, and that <i>BAP1</i><sup>+/-</sup> carriers have detectable serum levels of acetylated HMGB1 that further increase when they develop mesothelioma. We linked these findings to our discovery that BAP1 forms a trimeric protein complex with HMGB1 and with histone deacetylase 1 (HDAC1) that modulates HMGB1 acetylation and its release. Reduced BAP1 levels caused increased ubiquitylation and degradation of HDAC1, leading to increased acetylation of HMGB1 and its active secretion that in turn promoted mesothelial cell transformation.

  • Bai F
  • Barbour H
  • Bononi A
  • Carbone M
  • Gaudino G
  • Giorgi C
  • Haglund E
  • Kricek F
  • Minaai M
  • Morris P
  • Novelli F
  • Onuchic JN
  • Pass HI
  • Pastorino S
  • Patergnani S
  • Pinton P
  • Sakamoto G
  • Suarez JS
  • Takanishi Y
  • Tanji M
  • Wang Q
  • Xu R
  • Yang H
PubMed ID
Appears In
Proc Natl Acad Sci U S A, 2021, 118 (48)