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911.
912.
Stephanie Spannl Tomasz Buhl Ioannis Nellas Salma A Zeidan K Venkatesan Iyer Helena Khaliullina Carsten Schultz Andr Nadler Natalie A Dye Suzanne Eaton 《The EMBO journal》2021,40(7)
The authors regret omitting the citation of a bioRxiv preprint study by preprint: Emmons‐Bell et al (2020), who independently discovered the role of ion channel‐dependent membrane depolarization for Smo membrane accumulation in the fly wing disc. This study used a different methodological approach and did not describe the mechanism of how membrane potential affects hedgehog signaling. The reference is herewith added. 相似文献
913.
R D Kalraiya S S Iyer A Chati N G Mehta 《Indian journal of biochemistry & biophysics》1990,27(6):460-463
A not well-appreciated but clinically important aspect of malignant tumours is their effects on distantly located host cells. The effects, termed paraneoplastic syndromes, also pose an intriguing mechanistic problem: how do malignant cells influence properties of host cells not in contact with them? Erythrocytes from the circulation of rats bearing intraperitoneal Yoshida ascites sarcoma exhibit higher agglutinability with concanavalin A (Con A) than the cells from normal animals. Since the tumour and the red cells are not in contact, the enhanced agglutinability of the latter is a paraneoplastic effect. The mechanism by which the tumour brings about this effect is investigated as a model for paraneoplastic syndromes. The cell-free ascites fluid is able to impart high agglutinability on cells from normal animals in vitro. Also, when injected intraperitoneally in normal animals, the ascites fluid is able to enhance the agglutinability of erythrocytes in circulation. Apparently the tumour produces a substance(s) that appears in the ascites fluid and is able to diffuse into circulation, explaining the mechanism by which it can reach distant sites. From the cell-free ascites fluid three fractions have been isolated that are active in vitro. Of these, only one showed activity in vivo. From this fraction, a glycoprotein has been purified to homogeneity that confers maximal Con A-agglutinability on normal erythrocytes at 8 x 10(-7)M, at which concentration 6,400 molecules bind per cell. The protein has a molecular weight of 600 kDa in the native state and a pI of 5.35. It is made up of 4 identical subunits of Mr 170,000. It is detected in the plasma of tumour-bearing but not normal rats.(ABSTRACT TRUNCATED AT 250 WORDS) 相似文献
914.
Usha Natraj K. S. N. Iyer Vijaya Raghavan Smita Mahale Jacintha Pereira 《Journal of biosciences》1990,15(4):341-350
The antigenecity of tryptic fragments of reduced and carboxymethylated chicken riboflavin carrier protein were studied. The
tryptic sites of the native riboflavin carrier protein bound to riboflavin were inaccessible. The molecular weight and the
elution profile on high performance liquid chromatography (TSK 545 DEAE) were unaltered at an enzyme to substrate ratio of
1:31. However, carboxymethylated riboflavin carrier protein could be cleaved into 3 or 4 fragments at an enzyme to substrate
ratio of 1:250 or 1:125. Chromatographic separation of the tryptic fragments on high pressure liquid chromatography (TSK 545
DEAE) revealed the presence of two fragments with different elution profiles but similar molecular weight 26 ±2 kDa. Only
one fragment (associated with peak 2) had the ability to displace chicken riboflavin carrier protein in an homologous chicken
riboflavin carrier protein radioimmunoassay. Thus, carboxymethylated ribotlavin carrier protein which does not compete with
chicken riboflavin carrier protein in the radioimmunoassay, on mild trypsinization generates a fragment which interacts with
chicken riboflavin carrier protein in radioimmunoassay. 相似文献