Medical Biology - Research Publications

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Author: FAIRLIE, W × Author: Strasser, Andreas × Start date: 2000 × Type: Journal Article ×

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    Membrane-bound Fas ligand only is essential for Fas-induced apoptosis
    Reilly, LAO ; Tai, L ; Lee, L ; Kruse, EA ; Grabow, S ; Fairlie, WD ; Haynes, NM ; Tarlinton, DM ; Zhang, J-G ; Belz, GT ; Smyth, MJ ; Bouillet, P ; Robb, L ; Strasser, A (NATURE PUBLISHING GROUP, 2009-10-01)
    Fas ligand (FasL), an apoptosis-inducing member of the TNF cytokine family, and its receptor Fas are critical for the shutdown of chronic immune responses and prevention of autoimmunity. Accordingly, mutations in their genes cause severe lymphadenopathy and autoimmune disease in mice and humans. FasL function is regulated by deposition in the plasma membrane and metalloprotease-mediated shedding. Here we generated gene-targeted mice that selectively lack either secreted FasL (sFasL) or membrane-bound FasL (mFasL) to resolve which of these forms is required for cell killing and to explore their hypothesized non-apoptotic activities. Mice lacking sFasL (FasL(Deltas/Deltas)) appeared normal and their T cells readily killed target cells, whereas T cells lacking mFasL (FasL(Deltam/Deltam)) could not kill cells through Fas activation. FasL(Deltam/Deltam) mice developed lymphadenopathy and hyper-gammaglobulinaemia, similar to FasL(gld/gld) mice, which express a mutant form of FasL that cannot bind Fas, but surprisingly, FasL(Deltam/Deltam) mice (on a C57BL/6 background) succumbed to systemic lupus erythematosus (SLE)-like autoimmune kidney destruction and histiocytic sarcoma, diseases that occur only rarely and much later in FasL(gld/gld) mice. These results demonstrate that mFasL is essential for cytotoxic activity and constitutes the guardian against lymphadenopathy, autoimmunity and cancer, whereas excess sFasL appears to promote autoimmunity and tumorigenesis through non-apoptotic activities.
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    Characterisation of a novel A1-specific monoclonal antibody
    Lang, MJ ; Brennan, MS ; O'Reilly, LA ; Ottina, E ; Czabotar, PE ; Whitlock, E ; Fairlie, WD ; Tai, L ; Strasser, A ; Herold, MJ (NATURE PUBLISHING GROUP, 2014-12)
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    BCL-XL and MCL-1 are the key BCL-2 family proteins in melanoma cell survival
    Lee, EF ; Harris, TJ ; Tran, S ; Evangelista, M ; Arulananda, S ; John, T ; Ramnac, C ; Hobbs, C ; Zhu, H ; Gunasingh, G ; Segal, D ; Behren, A ; Cebon, J ; Dobrovic, A ; Mariadason, JM ; Strasser, A ; Rohrbeck, L ; Haass, NK ; Herold, MJ ; Fairlie, WD (NATURE PUBLISHING GROUP, 2019-04-24)
    Malignant melanoma is one of the most difficult cancers to treat due to its resistance to chemotherapy. Despite recent successes with BRAF inhibitors and immune checkpoint inhibitors, many patients do not respond or become resistant to these drugs. Hence, alternative treatments are still required. Due to the importance of the BCL-2-regulated apoptosis pathway in cancer development and drug resistance, it is of interest to establish which proteins are most important for melanoma cell survival, though the outcomes of previous studies have been conflicting. To conclusively address this question, we tested a panel of established and early passage patient-derived cell lines against several BH3-mimetic drugs designed to target individual or subsets of pro-survival BCL-2 proteins, alone and in combination, in both 2D and 3D cell cultures. None of the drugs demonstrated significant activity as single agents, though combinations targeting MCL-1 plus BCL-XL, and to a lesser extent BCL-2, showed considerable synergistic killing activity that was elicited via both BAX and BAK. Genetic deletion of BFL-1 in cell lines that express it at relatively high levels only had minor impact on BH3-mimetic drug sensitivity, suggesting it is not a critical pro-survival protein in melanoma. Combinations of MCL-1 inhibitors with BRAF inhibitors also caused only minimal additional melanoma cell killing over each drug alone, whilst combinations with the proteasome inhibitor bortezomib was more effective in multiple cell lines. Our data show for the first time that therapies targeting specific combinations of BCL-2 pro-survival proteins, namely MCL-1 plus BCL-XL and MCL-1 plus BCL-2, could have significant benefit for the treatment of melanoma.
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    The role of BH3-only protein Bim extends beyond inhibiting Bcl-2-like prosurvival proteins
    Merino, D ; Giam, M ; Hughes, PD ; Siggs, OM ; Heger, K ; O'Reilly, LA ; Adams, JM ; Strasser, A ; Lee, EF ; Fairlie, WD ; Bouillet, P (ROCKEFELLER UNIV PRESS, 2009-08-10)
    Proteins of the Bcl-2 family are critical regulators of apoptosis, but how its BH3-only members activate the essential effectors Bax and Bak remains controversial. The indirect activation model suggests that they simply must neutralize all of the prosurvival Bcl-2 family members, whereas the direct activation model proposes that Bim and Bid must activate Bax and Bak directly. As numerous in vitro studies have not resolved this issue, we have investigated Bim's activity in vivo by a genetic approach. Because the BH3 domain determines binding specificity for Bcl-2 relatives, we generated mice having the Bim BH3 domain replaced by that of Bad, Noxa, or Puma. The mutants bound the expected subsets of prosurvival relatives but lost interaction with Bax. Analysis of the mice showed that Bim's proapoptotic activity is not solely caused by its ability to engage its prosurvival relatives or solely to its binding to Bax. Thus, initiation of apoptosis in vivo appears to require features of both models.