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Volume 42 Issue 8, August 2010

Editorial

  • A group of medical geneticists from the countries bordering the Mediterranean Sea are seeking support for an enduring cooperative research structure. Their research productivity and ability to collaborate are both proven. The expected value of the proposed organization is high.

    Editorial

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Commentary

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News & Views

  • A new study reports that androgen signaling induces DNA double-strand breaks and TMPRSS2-ERG rearrangements through androgen receptor–mediated recruitment of topoisomerase 2B. These findings shed light on the generation of the most common fusion oncogene in human cancer.

    • Jiri Bartek
    • Petra Hamerlik
    • Jiri Lukas
    News & Views
  • A new study finds that individuals with high plasma triglyceride levels carry approximately twice as many rare, coding genetic variants within four candidate genes identified through genome-wide association studies than individuals without these high levels. This study demonstrates the overlap of rare and common variant signals at loci associated with lipid levels and shows the value of efforts to extend susceptibility variant discovery to embrace the full allele-frequency spectrum.

    • Anna L Gloyn
    • Mark I McCarthy
    News & Views
  • A new study reports that susceptibility to drug-induced liver injury by the cyclooxygenase 2 (COX-2) inhibitor lumiracoxib is associated with a human lymphocyte antigen (HLA) class II haplotype. This finding suggests that those at risk of hepatotoxicity can be identified by HLA genotyping, raising the possibility that lumiracoxib can be resurrected as a useful drug.

    • Guruprasad P Aithal
    • Ann K Daly
    News & Views
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Research Highlights

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Brief Communication

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Article

  • Srinivasan Yegnasubramanian and colleagues show that androgen signaling promotes recruitment of androgen receptor and TOP2B to sites of TMPRSS2-ERG genomic breakpoints, triggering TOP2B-mediated double-strand breaks. These findings provide insights into the mechanism underlying this common prostate cancer gene fusion event.

    • Michael C Haffner
    • Martin J Aryee
    • Srinivasan Yegnasubramanian
    Article
  • Thomas Bugge and colleagues report that the matriptase protease initiates an epidermal kallikrein proteolytic cascade in mice lacking Spink5, which encodes the serine protease inhibitor LEKTI. Loss of matriptase rescued some features of excessive proteolytic degradation of corneodesmosomes and inflammatory activation in LEKTI-deficient mice, which are a model of human Netherton syndrome.

    • Katiuchia Uzzun Sales
    • Andrius Masedunskas
    • Thomas H Bugge
    Article
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Letter

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Erratum

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