195 research outputs found

    MSH2/MSH6 Complex Promotes Error-Free Repair of AID-Induced dU:G Mispairs as well as Error-Prone Hypermutation of A:T Sites

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    Mismatch repair of AID-generated dU:G mispairs is critical for class switch recombination (CSR) and somatic hypermutation (SHM) in B cells. The generation of a previously unavailable Msh2āˆ’/āˆ’Msh6āˆ’/āˆ’ mouse has for the first time allowed us to examine the impact of the complete loss of MutSĪ± on lymphomagenesis, CSR and SHM. The onset of T cell lymphomas and the survival of Msh2āˆ’/āˆ’Msh6āˆ’/āˆ’ and Msh2āˆ’/āˆ’Msh6āˆ’/āˆ’Msh3āˆ’/āˆ’ mice are indistinguishable from Msh2āˆ’/āˆ’ mice, suggesting that MSH2 plays the critical role in protecting T cells from malignant transformation, presumably because it is essential for the formation of stable MutSĪ± heterodimers that maintain genomic stability. The similar defects on switching in Msh2āˆ’/āˆ’, Msh2āˆ’/āˆ’Msh6āˆ’/āˆ’ and Msh2āˆ’/āˆ’Msh6āˆ’/āˆ’Msh3āˆ’/āˆ’ mice confirm that MutSĪ± but not MutSĪ² plays an important role in CSR. Analysis of SHM in Msh2āˆ’/āˆ’Msh6āˆ’/āˆ’ mice not only confirmed the error-prone role of MutSĪ± in the generation of strand biased mutations at A:T bases, but also revealed an error-free role of MutSĪ± when repairing some of the dU:G mispairs generated by AID on both DNA strands. We propose a model for the role of MutSĪ± at the immunoglobulin locus where the local balance of error-free and error-prone repair has an impact in the spectrum of mutations introduced during Phase 2 of SHM

    Novel role for the transient receptor potential channel TRPM2 in prostate cancer cell proliferation

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    We have identified a novel function for a member of the transient receptor potential (TRP) protein super-family, TRPM2, in prostate cancer cell proliferation. TRPM2 encodes a non-selective cation-permeable ion channel. We found that selectively knocking down TRPM2 with the small interfering RNA technique inhibited the growth of prostate cancer cells but not of non-cancerous cells. The subcellular localization of this protein is also remarkably different between cancerous and non-cancerous cells. In BPH-1 (benign), TRPM2 protein is homogenously located near the plasma membrane and in the cytoplasm, whereas in the cancerous cells (PC-3 and DU-145), a significant amount of the TRPM2 protein is located in the nuclei in a clustered pattern. Furthermore, we have found that TRPM2 inhibited nuclear ADP-ribosylation in prostate cancer cells. However, TRPM2 knockdown-induced inhibition of proliferation is independent of the activity of poly(ADP-ribose) polymerases. We conclude that TRPM2 is essential for prostate cancer cell proliferation and may be a potential target for the selective treatment of prostate cancer

    Global Sustainability Under Uncertainty: How Do Multinationals Craft Regulatory Policies?

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    Multinational corporations are increasingly mindful of the significance of sustainability transitions and the need for operations that are energy efficient and environmentally sound. Achieving sustainability under conditions of uncertainty entails the involvement of multiple stakeholders in initiating and carrying outsustainability-focused initiatives. Using longitudinal analysis of Royal Dutch Shellā€™s sustainability policies, we developed an integrated model to elucidate how uncertainty influences sustainability policies in the specific context of multinational corporations (hereinafter ā€“ MNCs). We identified three phases in theevolution of Shellā€™s sustainability innovation: a self-reflective phase (2000ā€“2003) characterized by intense pressure from climate advocacy groups, an investment phase (2004ā€“2006) for which the MNC attempted to rise to the waste disposal and pollution challenge through renewable sources of energy, and a reorganization phase (2007ā€“2010) to streamline operations. We also uncovered themes that influence how regulatory policies are crafted: responding positively to the ā€œcommunityā€™s voiceā€, risk spreading through joint ventures, revenue transparency for government accountability and reporting innovation that confronts hard truths. The practical implications are outlined

    Understanding the market for justice

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    Trends in template/fragment-free protein structure prediction

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    Predicting the structure of a protein from its amino acid sequence is a long-standing unsolved problem in computational biology. Its solution would be of both fundamental and practical importance as the gap between the number of known sequences and the number of experimentally solved structures widens rapidly. Currently, the most successful approaches are based on fragment/template reassembly. Lacking progress in template-free structure prediction calls for novel ideas and approaches. This article reviews trends in the development of physical and specific knowledge-based energy functions as well as sampling techniques for fragment-free structure prediction. Recent physical- and knowledge-based studies demonstrated that it is possible to sample and predict highly accurate protein structures without borrowing native fragments from known protein structures. These emerging approaches with fully flexible sampling have the potential to move the field forward
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