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Xu L  Wei Y  Reboul J  Vaglio P  Shin TH  Vidal M  Elledge SJ  Harper JW 《Nature》2003,425(6955):316-321
Programmed destruction of regulatory proteins through the ubiquitin-proteasome system is a widely used mechanism for controlling signalling pathways. Cullins are proteins that function as scaffolds for modular ubiquitin ligases typified by the SCF (Skp1-Cul1-F-box) complex. The substrate selectivity of these E3 ligases is dictated by a specificity module that binds cullins. In the SCF complex, this module is composed of Skp1, which binds directly to Cul1, and a member of the F-box family of proteins. F-box proteins bind Skp1 through the F-box motif, and substrates by means of carboxy-terminal protein interaction domains. Similarly, Cul2 and Cul5 interact with BC-box-containing specificity factors through the Skp1-like protein elongin C. Cul3 is required for embryonic development in mammals and Caenorhabditis elegans but its specificity module is unknown. Here we report the identification of a large family of BTB-domain proteins as substrate-specific adaptors for C. elegans CUL-3. Biochemical studies using the BTB protein MEL-26 and its genetic target MEI-1 (refs 12, 13) indicate that BTB proteins merge the functional properties of Skp1 and F-box proteins into a single polypeptide.  相似文献   

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Jagasia R  Grote P  Westermann B  Conradt B 《Nature》2005,433(7027):754-760
Genetic analyses in Caenorhabditis elegans have been instrumental in the elucidation of the central cell-death machinery, which is conserved from C. elegans to mammals. One possible difference that has emerged is the role of mitochondria. By releasing cytochrome c, mitochondria are involved in the activation of caspases in mammals. However, there has previously been no evidence that mitochondria are involved in caspase activation in C. elegans. Here we show that mitochondria fragment in cells that normally undergo programmed cell death during C. elegans development. Mitochondrial fragmentation is induced by the BH3-only protein EGL-1 and can be blocked by mutations in the bcl-2-like gene ced-9, indicating that members of the Bcl-2 family might function in the regulation of mitochondrial fragmentation in apoptotic cells. Mitochondrial fragmentation is independent of CED-4/Apaf-1 and CED-3/caspase, indicating that it occurs before or simultaneously with their activation. Furthermore, DRP-1/dynamin-related protein, a key component of the mitochondrial fission machinery, is required and sufficient to induce mitochondrial fragmentation and programmed cell death during C. elegans development. These results assign an important role to mitochondria in the cell-death pathway in C. elegans.  相似文献   

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利用分担集合的思想证明了定理:设F是单位圆盘内的一族全纯函数族,a1和a2是2个不同的有限复数且a1+a2≠0;当α≥1时。如果对于任意的f∈F,Ef(S)=Ef′(s),S={a1,a2}在单位圆内成立,那么f是一个α-正规函数.  相似文献   

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A mechanism for synergistic activation of a mammalian gene by GAL4 derivatives   总被引:70,自引:0,他引:70  
M Carey  Y S Lin  M R Green  M Ptashne 《Nature》1990,345(6273):361-364
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In diverse organisms, calorie restriction slows the pace of ageing and increases maximum lifespan. In the budding yeast Saccharomyces cerevisiae, calorie restriction extends lifespan by increasing the activity of Sir2 (ref. 1), a member of the conserved sirtuin family of NAD(+)-dependent protein deacetylases. Included in this family are SIR-2.1, a Caenorhabditis elegans enzyme that regulates lifespan, and SIRT1, a human deacetylase that promotes cell survival by negatively regulating the p53 tumour suppressor. Here we report the discovery of three classes of small molecules that activate sirtuins. We show that the potent activator resveratrol, a polyphenol found in red wine, lowers the Michaelis constant of SIRT1 for both the acetylated substrate and NAD(+), and increases cell survival by stimulating SIRT1-dependent deacetylation of p53. In yeast, resveratrol mimics calorie restriction by stimulating Sir2, increasing DNA stability and extending lifespan by 70%. We discuss possible evolutionary origins of this phenomenon and suggest new lines of research into the therapeutic use of sirtuin activators.  相似文献   

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Lu R  Maduro M  Li F  Li HW  Broitman-Maduro G  Li WX  Ding SW 《Nature》2005,436(7053):1040-1043
The worm Caenorhabditis elegans is a model system for studying many aspects of biology, including host responses to bacterial pathogens, but it is not known to support replication of any virus. Plants and insects encode multiple Dicer enzymes that recognize distinct precursors of small RNAs and may act cooperatively. However, it is not known whether the single Dicer of worms and mammals is able to initiate the small RNA-guided RNA interference (RNAi) antiviral immunity as occurs in plants and insects. Here we show complete replication of the Flock house virus (FHV) bipartite, plus-strand RNA genome in C. elegans. We show that FHV replication in C. elegans triggers potent antiviral silencing that requires RDE-1, an Argonaute protein essential for RNAi mediated by small interfering RNAs (siRNAs) but not by microRNAs. This immunity system is capable of rapid virus clearance in the absence of FHV B2 protein, which acts as a broad-spectrum RNAi inhibitor upstream of rde-1 by targeting the siRNA precursor. This work establishes a C. elegans model for genetic studies of animal virus-host interactions and indicates that mammals might use a siRNA pathway as an antiviral response.  相似文献   

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分担值与亚纯函数的正规性   总被引:1,自引:0,他引:1  
把亚纯函数的分担值和推广了的球面导数相结合,得到了如下结果:设F是区域D内的亚纯函数族,若F中的任意函数,(∈F)的零点重数至少是k(k是正整数),f=0当且仅当f(k)=0,且当z∈E(1,f(k))时,存在正整数M(<1),使得|f(k)(z)|/1+|f(z)|k+1≤M 则F在D内正规.  相似文献   

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Raizen DM  Zimmerman JE  Maycock MH  Ta UD  You YJ  Sundaram MV  Pack AI 《Nature》2008,451(7178):569-572
There are fundamental similarities between sleep in mammals and quiescence in the arthropod Drosophila melanogaster, suggesting that sleep-like states are evolutionarily ancient. The nematode Caenorhabditis elegans also has a quiescent behavioural state during a period called lethargus, which occurs before each of the four moults. Like sleep, lethargus maintains a constant temporal relationship with the expression of the C. elegans Period homologue LIN-42 (ref. 5). Here we show that quiescence associated with lethargus has the additional sleep-like properties of reversibility, reduced responsiveness and homeostasis. We identify the cGMP-dependent protein kinase (PKG) gene egl-4 as a regulator of sleep-like behaviour, and show that egl-4 functions in sensory neurons to promote the C. elegans sleep-like state. Conserved effects on sleep-like behaviour of homologous genes in C. elegans and Drosophila suggest a common genetic regulation of sleep-like states in arthropods and nematodes. Our results indicate that C. elegans is a suitable model system for the study of sleep regulation. The association of this C. elegans sleep-like state with developmental changes that occur with larval moults suggests that sleep may have evolved to allow for developmental changes.  相似文献   

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H R Horvitz  P W Sternberg 《Nature》1991,351(6327):535-541
Developmental, genetic and molecular studies indicate that multiple intercellular signalling systems interact to specify the types and spatial patterns of cells generated during the formation of the vulva of the nematode Caenorhabditis elegans. Two classes of evolutionarily conserved transmembrane receptors and a Ras protein function in these signalling systems. The biology of vulval development provides a framework for understanding how cell interactions control the development of animals as diverse as nematodes, insects and mammals.  相似文献   

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设F为区域D上的一族亚纯函数,所有的零点重级至少是k,b为有穷非零复数,n,k为两正整数,P是有三个互相判别的零点的多项式.如果任意函数f,g∈F,P(f)(fn)(k)和P(g)(gn)(k)在D内分担b,则F在D内正规.  相似文献   

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研究了分担连续函数的全纯函数族的正规性问题,推广了一些已有的结论.设F为定义在区域D上的全纯函数族,h1,h2为两个连续函数满足对_z∈D有h1(z)≠h2(z),并设k≥2为正整数.若f∈F,有f(z)=hi(z)=〉|f(k)(z)|≤|hi(z)|,i=1,2,则F为D上的正规族;并举例说明了k=1时,结论不成立.此外,还将分担值条件用拓扑度条件代替得到了一个涉及拓扑度条件的全纯函数族正规定则.  相似文献   

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Fukui Y  Hashimoto O  Sanui T  Oono T  Koga H  Abe M  Inayoshi A  Noda M  Oike M  Shirai T  Sasazuki T 《Nature》2001,412(6849):826-831
Cell migration is a fundamental biological process involving membrane polarization and cytoskeletal dynamics, both of which are regulated by Rho family GTPases. Among these molecules, Rac is crucial for generating the actin-rich lamellipodial protrusion, a principal part of the driving force for movement. The CDM family proteins, Caenorhabditis elegans CED-5, human DOCK180 and Drosophila melanogaster Myoblast City (MBC), are implicated to mediate membrane extension by functioning upstream of Rac. Although genetic analysis has shown that CED-5 and Myoblast City are crucial for migration of particular types of cells, physiological relevance of the CDM family proteins in mammals remains unknown. Here we show that DOCK2, a haematopoietic cell-specific CDM family protein, is indispensable for lymphocyte chemotaxis. DOCK2-deficient mice (DOCK2-/-) exhibited migration defects of T and B lymphocytes, but not of monocytes, in response to chemokines, resulting in several abnormalities including T lymphocytopenia, atrophy of lymphoid follicles and loss of marginal-zone B cells. In DOCK2-/- lymphocytes, chemokine-induced Rac activation and actin polymerization were almost totally abolished. Thus, in lymphocyte migration DOCK2 functions as a central regulator that mediates cytoskeletal reorganization through Rac activation.  相似文献   

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主要得到了以下结果:设是一族平面区域D内的亚纯函数,a,b为有穷非零复数,k为大于1的整数.如果对于F中的任一元素f,满足f-a的零点重数至少为k,f(z)=a■f(k)(z)=a,f(k)(z)=b■f(k+1)(z)=b,则当k≥3时,F为正规族,k=2并且a/b≠4时,F为正规族.并且给出了1个例子说明条件a/b≠4是必要的.  相似文献   

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