C1QA Blocking Peptide

Price:

216.14 €

Known as:: C1QA Blocking Peptide
Catalog number:: 33r-7113
Product Quantity:: USD
Category:: -
Supplier:: Fitzgerald industries international
Gene target:: C1QA Blocking Peptide

Related genes to: C1QA Blocking Peptide

Gene:: C1QA ^{NIH gene}
Name:: complement C1q A chain
Previous symbol:: -
Synonyms:: -
Chromosome:: 1p36.12
Locus Type:: gene with protein product
Date approved:: 2001-06-22
Date modifiied:: 2019-04-23

Related products to: C1QA Blocking Peptide

α - Calcitonin Gene Related Peptide, α - CGRP, rat&_945;2&_946;1 Integrin Ligand Peptide&_946;_catenin peptide(Ala92)-Peptide 6 98% C93H155N31O26 CAS:(Arg)9 Peptide (Arg8)-Vasopressin Biotin peptide This is (Arg8)-Vasopressin Biotin peptide. For research use only.(Asn5)-Delta-Sleep Inducing Peptide (Asn5)-Delta-Sleep Inducing Peptide (rabbit), (Asn5)-DSIP (rabbit) 98% C35H49N11O14 CAS: 80064-67-1(Asn5)_Delta_Sleep Inducing Peptide Salt _ Binding _ Synonym (Asn5)_Delta_Sleep Inducing Peptide (rabbit), (Asn5)_DSIP (rabbit) SumFormula C35H49N11O14(Asn5)_Delta_Sleep Inducing Peptide Salt _ Binding _ Synonym (Asn5)_Delta_Sleep Inducing Peptide (rabbit), (Asn5)_DSIP (rabbit) SumFormula C35H49N11O14(Biotin Conjugates) Dopamine D2 Receptor Immunogen: peptide Host: Rabbit(Biotin Conjugates) Glucose Transporter 1 Immunogen: peptide Host: Rabbit(Biotin Conjugates) PDE3A(goat) Immunogen: peptide Host: Rabbit(Biotin Conjugates) PDE7A(Goat) Immunogen: peptide (23mer) Host: Rabbit(Biotin Conjugates) Phospho-calcium channel 2A subunit Immunogen: peptide Host: Rabbit(Biotin Conjugates) Phospho-cyclic 5'-nucleotidase Immunogen: peptide Host: Rabbit

Related articles to: C1QA Blocking Peptide

Single-cell transcriptomic profiling uncovers key molecular signatures in glioma pathogenesis.
Glioma represents the most prevalent and lethal primary malignant tumor of the central nervous system, characterized by remarkable cellular heterogeneity and poor prognosis. Comprehensive characterization of glioma at single-cell resolution is essential for identifying novel therapeutic targets and improving patient outcomes. - Source: PubMed
Publication date: 2026/05/28
Gu ChengcongWu XiaojinYang Liang
Plasma proteomics improves risk prediction in heart failure and reveals unique biology in chronic chagas cardiomyopathy.
Chronic Chagas cardiomyopathy (CCC) remains a major cause of heart failure (HF)-related mortality in Latin America and is increasingly recognized as a global health concern. Prognostic models developed in non-Chagas populations often perform poorly in CCC, highlighting the need for etiology-specific risk stratification. - Source: PubMed
Publication date: 2026/06/08
Patané José S LGiugni Fernando RRosa Rogério SMarcondes-Braga Fabiana GMansur Alfredo JPereira Alexandre CKrieger Jose E
Genetic landscape of early-onset systemic lupus erythematous in India.
To investigate the genetic basis of early-onset systemic lupus erythematosus (EOSLE) in a large Indian pediatric SLE (pSLE) cohort. - Source: PubMed
Sharma MadhubalaPilania Rakesh KumarVolpi StefanoBocca PaolaJindal AnkurVignesh PandiarajanSuri DeeptiSharma SaniyaDhaliwal ManpreetGarg RavinderKaur GurjitSaka RuchiMamadpur MahabaleshwarMahadevan SabarinathHaque IsrarulGhosh ParasarReddy MounikaChoudhary AbhijitArora AmitDas ReenaAhluwalia JasminaGattorno MarcoSingh SurjitRawat Amit
Single-cell-based analysis establishes C1QA-mediated promotion of high glucose-induced tubular epithelial injury via ERS in DN.
Diabetic nephropathy (DN) poses a growing worldwide health challenge as a leading cause of end-stage renal disease, a condition that arises from a complex, poorly defined pathophysiology. Endoplasmic reticulum stress (ERS) is recognized as a pivotal contributor to renal cell injury in DN. While complement component C1q A chain (C1QA) is integral to innate immunity, its specific role and mechanism in DN, particularly in relation to ERS, remain unexplored. - Source: PubMed
Publication date: 2026/06/03
Zhang XiaoyingLi LeiZhang FengjiaoZhu MengluKang ZhiqiangMao Yu
Single-cell and spatial transcriptomics reveal Thbs1-CD36 crosstalk between Kupffer and hepatic stellate cells following mesenchymal stem cell-derived small extracellular vesicles transplantation, alleviating liver fibrosis.
Small extracellular vesicles (sEVs) derived from mesenchymal stem cells represent a novel regenerative therapeutic strategy for various liver injuries. Menstrual blood-derived mesenchymal stem cells (MenSCs)-derived EVs may have therapeutic potential in treating liver fibrosis. In this study, systemically injected MenSCs-derived sEVs migrated into the injured liver, ameliorated serological indices, and decreased collagenous fiber accumulation in carbon tetrachloride (CCl)-induced liver fibrosis mouse models. We aimed to explore the underlying mechanism for the therapeutic effect of MenSC-sEVs. - Source: PubMed
Publication date: 2026/05/28
Chen LijunZhang NingHuang YuqiQu JingjingFang YangxinYuan YinFu JiaminWan DalongZhang QiChen LuWen ZuoshiChen XinYuan LiXu ZhenyuLi YifeiHu ChenxiaYan HuadongIzawa HiromiYoshimoto TakayukiLi LanjuanXiang Charlie

C1QA Blocking Peptide

Related genes to: C1QA Blocking Peptide

Related products to: C1QA Blocking Peptide

Related articles to: C1QA Blocking Peptide

Single-cell transcriptomic profiling uncovers key molecular signatures in glioma pathogenesis.

Plasma proteomics improves risk prediction in heart failure and reveals unique biology in chronic chagas cardiomyopathy.

Genetic landscape of early-onset systemic lupus erythematous in India.

Single-cell-based analysis establishes C1QA-mediated promotion of high glucose-induced tubular epithelial injury via ERS in DN.

Single-cell and spatial transcriptomics reveal Thbs1-CD36 crosstalk between Kupffer and hepatic stellate cells following mesenchymal stem cell-derived small extracellular vesicles transplantation, alleviating liver fibrosis.