Advanced oxidation protein products trigger apoptosis and block epithelial-to-mesenchymal transition in crypt epithelial cells.

Advanced oxidation protein products (AOPPs) are uremic toxins. The present study aimed to investigate the effects of AOPPs on the epithelial mesenchymal transition (EMT) and apoptosis of rat crypt epithelial cells, and to assess the signaling pathways involved. The oxidized rat serum albumin was obtained by sodium hypochlorite modification as AOPPs, and the rat serum albumin (RSA) without sodium hypochlorite modification was set as the control.

A microporous metal-organic framework containing an exceptional four-connecting 4(2)6(4) topology and a combined effect for highly selective adsorption of CO2 over N2.

Reported here is a new microporous metal-organic framework, namely [Zn(2)(L)(btc)(Hbtc)] [NH(2)(CH(3))(2)]·(DMF)(2)(H(2)O)(4) (1), which is synthesized solvo(hydro)thermally by the self-assembly of Zn(NO(3))(2), N(4),N(4)-di(pyridin-3-yl)-[1,1'-biphenyl]-4,4'-dicarboxamide (L) and 1,3,5-benzenetricarboxylate acid (H(3)btc). Its topology can be described as a four-connecting 4(2)6(4) matrix containing both tetrahedral metal and ligand nodes. Interestingly, such a matrix has the same topology symbol as that observed in the well known sodalite (SOD) net, but the td10 of 434 is different from the td10 of 791 for the SOD net, indicative of an exceptional four-connecting 4(2)6(4) net.

Solvent-induced supramolecular isomers, structural diversity, and unprecedented in situ formation of both inorganic and organic ions in inorganic-organic mercury(II) complexes.

Reported here is, for the first time, an important study of solvent effect on structural diversity in inorganic-organic mercury(II) complexes. As a result, the first supramolecular isomer in mercury(II) complexes is obtained. Importantly, a previously unobserved in situ generation of both inorganic (Cl(-)) and organic ([CH(3)-L1-CH(3)](2+)) ions was also observed.

A self-catenated network containing unprecedented 0D + 2D → 2D polycatenation array.

Herein, we report a new acylamide ligand and its application in the construction of a metal-organic framework. The resultant acylamide metal-organic framework, namely [Zn(2)(L)(OH)(btc)](n) (1, L = N(1),N(4)-bis(pyridin-3-ylmethyl) naphthalene-1,4-dicarboxamide, H(3)btc = benzene-1,3,5-tricarboxylic acid), was obtained by hydrothermal synthesis. The outstanding structural feature of it is the 0D + 2D → 2D polycatenation array containing a self-catenated feature which has never previously been observed.

A series of 1D Dy(III) compound showing slow magnetic relaxation: synthesis, structure, and magnetic studies.

In this work, we present the synthesis, structure, and magnetic studies of three 1D homo-spin Dy(III) compounds in detail. For 1, one crystallography-independent Dy(III) site is contained and the coordination surrounding is a distorted square-antiprism geometry. Within 2, four crystallography-independent Dy(III) sites with largely distorted square-antiprism geometry are observed.

[Pattern of lymph node metastasis and extent of lymphadenectomy for distal gastric cancer].

Objective: To analyze lymph node (LN) metastasis patterns and determine the appropriate extent of LN dissection in distal-third gastric cancer.

Methods: Clinical data of 545 patients with distal third gastric cancer undergoing radical operation in the Fujian Provincial Hospital between 2001 and 2010 were analyzed retrospectively. The metastasis rate for each LN station was analyzed stratified by the depth of tumor invasion.

Chiral 1D Dy(III) compound showing slow magnetic relaxation.

Herein, we present one chiral Dy(III) compound, namely Dy(L)(3)(1, HL = 2-methylbenzoic acid), synthesized from the achiral HL ligand. Within 1, along a direction the seven-coordinated Dy(III) ion are bridged by double L carboxylate and single L oxygen to give rise to the 1D helical chain. The magnetic studies suggest small intra-chain ferromagnetic interactions.

[Effect of polydatin on lipopolysaccharide-induced leucocyte chemotaxis].

Objective: To understand the action mechanisms of polydatin (PD) in the treatment of septic shock in view of its effect on lipopolysaccharide (LPS)-induced chemotaxis of the leucocytes.

Method: Chemotactic chamber assay was used to investigate the regulative role of PD in chemotaxis of the neutrophils in response to LPS stimulation.

Results: The chemotactic index of normal neutrophils was 4.

Protective effect of polydatin against lipopolysaccharide-induced myocardial injury.

Objective: To observe the effect of lipopolysaccharide (LPS) on actin cytoskeleton of rat cardiac myocytes and the intervention effect of polydatin against this effect.

Methods: Rat cardiac myocytes were isolated from newborn SD rats (3 days old) and cultured in vitro, which were then divided into control group (treated with D-Hank's solution for 30 min), polydatin group (with 0.2 mmol/L polydatin treatment for 10 min), LPS group (with 100 ng/ml LPS stimulation for 30 min), and LPS/polydatin group (with 100 ng/ml LPS stimulation for 30 min followed by incubation with 0.