Electrical and band-gap properties of amorphous zinc-indium-tin oxide thin films

Zinc-indium-tin oxide (ZITO) films were grown by pulsed-laser deposition.Three different material compositions were investigated:ZITO-30,ZITO-50 and ZITO-70 in which 30％,50％ and 70％,respectively,of the...     

SO_2两转两吸流程中“ⅢⅠ-ⅣⅡ”和“ⅢⅡ-ⅣⅠ”换热情况浅析

通过工艺计算，定量分析比较 Ｓ Ｏ２ 转化中“ⅢⅠ－ ⅣⅡ”和“ⅢⅡ－ ⅣⅠ”两种换热流程的差异，论证了就换热情况而言，“ⅢⅠ－ ⅣⅡ”流程优于“ⅢⅡ－ ⅣⅠ”流程     

用柱层析和TLC分离小麦PGIP和植保素

植物抗病能力大小的测定需要比较准确可靠且相对简便的办法。采用接种病菌于植物上观察染菌情况虽然直观，但受病菌本身的生理状态及外界环境影响很大，且不便于定量的表述。因此，选择合适的生理生化指标作为植物抗性大小的衡量标准，对于植物病理的研究具有重要的意义。选择了小麦体系的两种抗性物质－ 小麦植保素和 Ｐ Ｇ Ｉ Ｐ作为小麦的抗性指标来分离分析     

Structure of Cdc42 in complex with the GTPase-binding domain of the 'Wiskott-Aldrich syndrome' protein.

The Rho-family GTP-hydrolysing proteins (GTPases), Cdc42, Rac and Rho, act as molecular switches in signalling pathways that regulate cytoskeletal architecture, gene expression and progression of the cell cycle. Cdc42 and Rac transmit many signals through GTP-dependent binding to effector proteins containing a Cdc42/Rac-interactive-binding (CRIB) motif. One such effector, the Wiskott-Aldrich syndrome protein (WASP), is postulated to link activation of Cdc42 directly to the rearrangement of actin. Human mutations in WASP cause severe defects in haematopoletic cell function, leading to clinical symptoms of thrombocytopenia, immunodeficiency and eczema. Here we report the solution structure of a complex between activated Cdc42 and a minimal GTPase-binding domain (GBD) from WASP. An extended amino-terminal GBD peptide that includes the CRIB motif contacts the switch I, beta2 and alpha5 regions of Cdc42. A carboxy-terminal beta-hairpin and alpha-helix pack against switch II. The Phe-X-His-X2-His portion of the CRIB motif and the alpha-helix appear to mediate sensitivity to the nucleotide switch through contacts to residues 36-40 of Cdc42. Discrimination between the Rho-family members is likely to be governed by GBD contacts to the switch I and alpha5 regions of the GTPases. Structural and biochemical data suggest that GBD-sequence divergence outside the CRIB motif may reflect additional regulatory interactions with functional domains that are specific to individual effectors.