antibody+against+insulin Search Results

Menge	Bestellnummer	Bestellinformationen	St./Pkg.	Listenpreis
			96-Well Plate

Menge	Bestellnummer	Bestellinformationen	St./Pkg.	Listenpreis
	48-602MAG	Buffer Detection Kit for Magnetic Beads	1 Kit

Molecular analysis of non-small cell lung cancer identifies subsets with different sensitivity to insulin-like growth factor I receptor inhibition.

This study aimed to identify molecular determinants of sensitivity of non-small cell lung cancer (NSCLC) to anti-insulin-like growth factor receptor (IGF-IR) therapy.A total of 216 tumor samples were investigated, of which 165 consisted of retrospective analyses of banked tissue and an additional 51 were from patients enrolled in a phase II study of figitumumab, a monoclonal antibody against IGF-IR, in stage IIIb/IV NSCLC. Biomarkers assessed included IGF-IR, epidermal growth factor receptor, IGF-II, IGF-IIR, insulin receptor substrate 1 (IRS-1), IRS-2, vimentin, and E-cadherin. Subcellular localization of IRS-1 and phosphorylation levels of mitogen-activated protein kinase and Akt1 were also analyzed.IGF-IR was differentially expressed across histologic subtypes (P = 0.04), with highest levels observed in squamous cell tumors. Elevated IGF-IR expression was also observed in a small number of squamous cell tumors responding to chemotherapy combined with figitumumab (P = 0.008). Because no other biomarker/response interaction was observed using classical histologic subtyping, a molecular approach was undertaken to segment NSCLC into mechanism-based subpopulations. Principal component analysis and unsupervised Bayesian clustering identified three NSCLC subsets that resembled the steps of the epithelial to mesenchymal transition: E-cadherin high/IRS-1 low (epithelial-like), E-cadherin intermediate/IRS-1 high (transitional), and E-cadherin low/IRS-1 low (mesenchymal-like). Several markers of the IGF-IR pathway were overexpressed in the transitional subset. Furthermore, a higher response rate to the combination of chemotherapy and figitumumab was observed in transitional tumors (71%) compared with those in the mesenchymal-like subset (32%; P = 0.03). Only one epithelial-like tumor was identified in the phase II study, suggesting that advanced NSCLC has undergone significant dedifferentiation at diagnosis.NSCLC comprises molecular subsets with differential sensitivity to IGF-IR inhibition.
Dokumententyp:: Referenz
Produkbestellnummer:: 05-166
Produktbezeichnung:: Anti-IGF-II Antibody, clone S1F2

Localization and timing of appearance of insulin, insulin-like growth factor-I, and their receptors in the human fetal müllerian tract.

OBJECTIVE: The factors that regulate fetal müllerian tract development are still unknown. Insulin and insulin-like growth factor-I are peptides postulated to serve as autocrine or paracrine regulators of cell activity. We have previously demonstrated that messenger ribonucleic acid for insulin and insulin-like growth factor-I receptors are expressed in fetal uterine tissues. We undertook this study to determine by immunohistochemical techniques the exact location of these two growth factors and their receptors in the human fetal uterus. STUDY DESIGN: We obtained freshly discarded human fetal uteri (n = 12) between 15 and 22 weeks of gestation from elective pregnancy terminations. Frozen-section specimens were incubated with antibodies against insulin, insulin-like growth factor-I, insulin receptor, and insulin-like growth factor-I receptor. These sections were then incubated with a second antibody conjugated to fluorescein isothiocyanate and examined under phase and fluorescent microscopy. RESULTS: The fetal endometrium at 19 and 22 weeks of gestation contained insulin, insulin-like growth factor-I, insulin receptor, and insulin-like growth factor-I receptor. The distribution of immunofluorescence in the endometrium is similar for both insulin and its receptor. The same pattern of immunostaining was likewise demonstrated for insulin-like growth factor-I and its receptor. CONCLUSION: The localization of these growth factors and their receptors, combined with our previous messenger ribonucleic acid data, suggest an autocrine or paracrine role for insulin and insulin-like growth factor-I in the developing human fetal müllerian tract.

Dokumententyp:

Referenz

Produkbestellnummer:

05-172

Produktbezeichnung:

Anti-IGF-I Antibody, clone Sm1.2

Das Produkt wurde in Ihre Bestellung aufgenommen

antibody+against+insulin

Suche eingrenzen Grenzen Sie Ihre Suche mit den nachstehenden Filtern ein

Dokumententyp

Molecular analysis of non-small cell lung cancer identifies subsets with different sensitivity to insulin-like growth factor I receptor inhibition.

Localization and timing of appearance of insulin, insulin-like growth factor-I, and their receptors in the human fetal müllerian tract.

Wählen Sie eine Spezies	.
Wählen Sie eine Panelart	.
Wählen Sie ein Kit	.
Wählen Sie eine Probenart	Bei einigen Panels entscheidet die Probenart, welche Analyten zusammen analysiert werden können.

Spezies
Panelart
Gewähltes Kit

PRODUKTE Produkte nach Anwendung Produkte nach Marke Produkte nach Industrie Produkte nach Art Bestellungen	SUPPORT Hilfe Feedback Cookies Kundendienst & Technischer Support HÄUFIG GESTELLTE FRAGEN Patente Kontaktaufnahme	UNTERNEHMEN Über uns Neuigkeiten Veranstaltungen Karriere Land ändern	Forschung. Entwicklung. Produktion. Wir sind ein führender Anbieter für die globale Life-Science-Industrie: Lösungen und Dienstleistungen für die Forschung, Entwicklung und Produktion in der Biotechnologie und Pharmaindustrie.


Merck-Gruppe Impressum Nutzungsbedingungen Datenschutzerklärung Verkaufsbedingungen

© 2025 Merck KGaA, Darmstadt, Germany and/or its affiliates. All Rights Reserved.Cookie Settings