Bachem cortistatin mouse/rat cst-14

a Sequence comparison of human Somatostatin (SST) to rat, mouse and human Cortistatins (CST). b Backbone superposition of the 10-lowest energy conformers. The peptide backbone is shown in gold and the N- and C-terminus residues, as well as the disulfide bond are labelled. Representative aromatic clusters. All side chains are shown to facilitate structural analysis. Side chains participating in the interactions are specifically labelled. c Schematic representation of <t>Cortistatin-14</t> sequence. Positions Xa, Xb, Xc and Xd have been mutated to prepare the analogues. Native CST was also synthesised for the NMR and functional studies. Sequences of the analogues prepared in this work. Substitutions are coloured. Synthetic scheme is displayed as Supplementary Fig. . d Schematic representations of the relative affinities of SST, CST and analogues A2-A5 for the different Somatostatin receptors (SSTR1-SSTR5) Supplementary Fig. . The relative affinities are represented based on the determined IC 50 values. The values are collected as Supplementary Table .

Cortistatin Mouse/Rat Cst 14, supplied by Bachem, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/cortistatin mouse/rat cst-14/product/Bachem
Average 90 stars, based on 1 article reviews

cortistatin mouse/rat cst-14 - by Bioz Stars, 2026-04

90/100 stars

Buy from Supplier

mouse polyclonal primary antibodies against cerebroside sulfotransferase (cst) (Abnova)

Abnova mouse polyclonal primary antibodies against cerebroside sulfotransferase (cst)

Mouse Polyclonal Primary Antibodies Against Cerebroside Sulfotransferase (Cst), supplied by Abnova, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/mouse polyclonal primary antibodies against cerebroside sulfotransferase (cst)/product/Abnova
Average 90 stars, based on 1 article reviews

mouse polyclonal primary antibodies against cerebroside sulfotransferase (cst) - by Bioz Stars, 2026-04

90/100 stars

Buy from Supplier

mouse cst-29 (Bachem)

Bachem mouse cst-29

Mouse Cst 29, supplied by Bachem, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/mouse cst-29/product/Bachem
Average 90 stars, based on 1 article reviews

mouse cst-29 - by Bioz Stars, 2026-04

90/100 stars

Buy from Supplier

Image Search Results

Journal: Nature Communications

Article Title: Structure-based design of a Cortistatin analogue with immunomodulatory activity in models of inflammatory bowel disease

doi: 10.1038/s41467-021-22076-5

Figure Lengend Snippet: a Sequence comparison of human Somatostatin (SST) to rat, mouse and human Cortistatins (CST). b Backbone superposition of the 10-lowest energy conformers. The peptide backbone is shown in gold and the N- and C-terminus residues, as well as the disulfide bond are labelled. Representative aromatic clusters. All side chains are shown to facilitate structural analysis. Side chains participating in the interactions are specifically labelled. c Schematic representation of Cortistatin-14 sequence. Positions Xa, Xb, Xc and Xd have been mutated to prepare the analogues. Native CST was also synthesised for the NMR and functional studies. Sequences of the analogues prepared in this work. Substitutions are coloured. Synthetic scheme is displayed as Supplementary Fig. . d Schematic representations of the relative affinities of SST, CST and analogues A2-A5 for the different Somatostatin receptors (SSTR1-SSTR5) Supplementary Fig. . The relative affinities are represented based on the determined IC 50 values. The values are collected as Supplementary Table .

Article Snippet: Cortistatin (mouse/rat CST-14, Bachem) and its synthesised analogues were added at a concentration of 100 nM at the beginning of culture.

Techniques: Sequencing, Comparison, Analogues, Functional Assay

Effects of Somatostatin (SST), Cortistatin (CST) and analogue 5 (A5) on the production of inflammatory cytokines and nitric oxide by LPS-activated mouse Raw 264 macrophages ( a ), on cell proliferation and production of Th1-type cytokines by anti-CD3-activated mouse spleen cells ( b ) and on the production of Th2-type cytokines by OVA-activated spleen cells isolated from mice immunised with OVA ( c ). Peptides were used at 100 nM and the dose-response curve for analogue 5 and cortistatin are shown in Supplementary Fig. . Cells cultured in medium alone were used as unstimulated controls. Data are the mean ± SEM with dots representing individual values of biologically independent cell cultures, each performed in duplicate. Statistical significance between groups was assessed by paired, two-tailed Student’s t test. *** p < 0.001, **** p < 0.0001 vs. stimulated cells in the absence of peptides. Exact p -values are shown for p > 0.001. Source data are provided as a Source Data file.

Journal: Nature Communications

Article Title: Structure-based design of a Cortistatin analogue with immunomodulatory activity in models of inflammatory bowel disease

doi: 10.1038/s41467-021-22076-5

Figure Lengend Snippet: Effects of Somatostatin (SST), Cortistatin (CST) and analogue 5 (A5) on the production of inflammatory cytokines and nitric oxide by LPS-activated mouse Raw 264 macrophages ( a ), on cell proliferation and production of Th1-type cytokines by anti-CD3-activated mouse spleen cells ( b ) and on the production of Th2-type cytokines by OVA-activated spleen cells isolated from mice immunised with OVA ( c ). Peptides were used at 100 nM and the dose-response curve for analogue 5 and cortistatin are shown in Supplementary Fig. . Cells cultured in medium alone were used as unstimulated controls. Data are the mean ± SEM with dots representing individual values of biologically independent cell cultures, each performed in duplicate. Statistical significance between groups was assessed by paired, two-tailed Student’s t test. *** p < 0.001, **** p < 0.0001 vs. stimulated cells in the absence of peptides. Exact p -values are shown for p > 0.001. Source data are provided as a Source Data file.

Article Snippet: Cortistatin (mouse/rat CST-14, Bachem) and its synthesised analogues were added at a concentration of 100 nM at the beginning of culture.

Techniques: Isolation, Cell Culture, Two Tailed Test

a Protective effects against acute severe colitis induced by oral DSS by the treatment with Cortistatin (CST) and analogue 5 (A5) (as indicated in the scheme) evaluated by disease activity indexes (scoring body weight loss, stool consistency and presence of faecal blood), survival rate, macroscopic signs of colon inflammation (damage score, length and weight of colon) and histopathological scores. b Comparative therapeutic effects of treatments with A5 and anti-mouse TNFα antibody in a model of relapsing-remitting colitis induced by cyclic administration of DSS (see scheme for experimental design). c Effects of A5 and anti-TNFα treatments on levels of cytokines in colonic mucosa of mice with DSS-induced relapsing-remitting colitis. Mice receiving tap water instead of DSS were used as naive controls. Animals injected with saline instead of A5 were used as untreated colitic mice. n = 8 mice/group for all assays, unless for histological analysis ( n = 5 mice/group in panel a , and n = 3 mice/group in panel b , where representative images are shown at ×100 magnification, scale bar: 200 µm). Data are mean ± SEM with dots representing individual values of biologically independent animals. Statistical differences between groups were calculated using two-tailed non-parametric Mann–Whitney test (for disease activity index, colon damage and microscopic scores), unpaired two-tailed Student’s t test (for colon length and weight) and Kaplan–Meier test (for survival). *** p < 0.001; **** p < 0.0001 versus untreated DSS-colitic mice (saline). Exact p -values are shown for p > 0.001. Source data are provided as a Source Data file. i.p. intraperitoneal, s.c. subcutaneous, i.v. intravenous.

Journal: Nature Communications

Article Title: Structure-based design of a Cortistatin analogue with immunomodulatory activity in models of inflammatory bowel disease

doi: 10.1038/s41467-021-22076-5

Figure Lengend Snippet: a Protective effects against acute severe colitis induced by oral DSS by the treatment with Cortistatin (CST) and analogue 5 (A5) (as indicated in the scheme) evaluated by disease activity indexes (scoring body weight loss, stool consistency and presence of faecal blood), survival rate, macroscopic signs of colon inflammation (damage score, length and weight of colon) and histopathological scores. b Comparative therapeutic effects of treatments with A5 and anti-mouse TNFα antibody in a model of relapsing-remitting colitis induced by cyclic administration of DSS (see scheme for experimental design). c Effects of A5 and anti-TNFα treatments on levels of cytokines in colonic mucosa of mice with DSS-induced relapsing-remitting colitis. Mice receiving tap water instead of DSS were used as naive controls. Animals injected with saline instead of A5 were used as untreated colitic mice. n = 8 mice/group for all assays, unless for histological analysis ( n = 5 mice/group in panel a , and n = 3 mice/group in panel b , where representative images are shown at ×100 magnification, scale bar: 200 µm). Data are mean ± SEM with dots representing individual values of biologically independent animals. Statistical differences between groups were calculated using two-tailed non-parametric Mann–Whitney test (for disease activity index, colon damage and microscopic scores), unpaired two-tailed Student’s t test (for colon length and weight) and Kaplan–Meier test (for survival). *** p < 0.001; **** p < 0.0001 versus untreated DSS-colitic mice (saline). Exact p -values are shown for p > 0.001. Source data are provided as a Source Data file. i.p. intraperitoneal, s.c. subcutaneous, i.v. intravenous.

Article Snippet: Cortistatin (mouse/rat CST-14, Bachem) and its synthesised analogues were added at a concentration of 100 nM at the beginning of culture.

Techniques: Activity Assay, Injection, Saline, Two Tailed Test, MANN-WHITNEY

NMR restraints and ensemble of conformers corresponding to A 5 . a Side-chain amide region of the analogue 5 ( 1 H-NOESY experiment), with peak assignments. Amide/proton alpha (left) and amide/aromatic (right) regions of the analogue 5 ( 1 H-NOESY experiment), with peak assignments are shown as Supplementary Fig. . 1D set of dilution experiments are included as Supplementary Fig. . b Backbone superposition of the 15 lowest-energy calculated conformers. c Analogue 5 , lowest energy conformer. Side chains are depicted as sticks. The residues defining the aromatic cluster are shown in yellow, the octanoyl moiety is highlighted in green whereas the remaining residues are shown in blue. The peptide backbone is shown in white. On the right, the equivalent Cortistatin conformer for comparison (shown in Fig. ). d Side chain and backbone distribution for the ensemble of the 15 best conformers shown as two orientations. Some residues are labelled. e Comparison of the pharmacophore region of analogue 5 to that of Cortistatin conformations represented in Fig. . The comparison includes the distances between C-gamma atoms of the five residues considered to define the pharmacophore. The backbone and Chi1 comparison of these six molecules are provided as Supplementary Fig. . Distances are represented as ranges to include the distance dispersion in the ensemble of conformations.

Journal: Nature Communications

Article Title: Structure-based design of a Cortistatin analogue with immunomodulatory activity in models of inflammatory bowel disease

doi: 10.1038/s41467-021-22076-5

Figure Lengend Snippet: NMR restraints and ensemble of conformers corresponding to A 5 . a Side-chain amide region of the analogue 5 ( 1 H-NOESY experiment), with peak assignments. Amide/proton alpha (left) and amide/aromatic (right) regions of the analogue 5 ( 1 H-NOESY experiment), with peak assignments are shown as Supplementary Fig. . 1D set of dilution experiments are included as Supplementary Fig. . b Backbone superposition of the 15 lowest-energy calculated conformers. c Analogue 5 , lowest energy conformer. Side chains are depicted as sticks. The residues defining the aromatic cluster are shown in yellow, the octanoyl moiety is highlighted in green whereas the remaining residues are shown in blue. The peptide backbone is shown in white. On the right, the equivalent Cortistatin conformer for comparison (shown in Fig. ). d Side chain and backbone distribution for the ensemble of the 15 best conformers shown as two orientations. Some residues are labelled. e Comparison of the pharmacophore region of analogue 5 to that of Cortistatin conformations represented in Fig. . The comparison includes the distances between C-gamma atoms of the five residues considered to define the pharmacophore. The backbone and Chi1 comparison of these six molecules are provided as Supplementary Fig. . Distances are represented as ranges to include the distance dispersion in the ensemble of conformations.

Article Snippet: Cortistatin (mouse/rat CST-14, Bachem) and its synthesised analogues were added at a concentration of 100 nM at the beginning of culture.

Techniques: Comparison, Dispersion

mouse cst Search Results

Image Search Results