ORCID Profile
0000-0002-3554-7538
Current Organisation
Bonn-Rhein-Sieg University of Applied Sciences
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Publisher: Proceedings of the National Academy of Sciences
Date: 23-07-2019
Abstract: Plant sap-feeding insects thrive despite feeding exclusively on a diet lacking in essential amino acids. This nutritional deficit is countered through endosymbiotic relationships with microbial symbionts. Nonessential amino acids, vital for microbial symbionts, are utilized by symbiont metabolic pathways and yield essential amino acids required by their eukaryotic hosts. Symbionts are completely dependent on their host to meet nutritional requirements. The endosymbionts are surrounded in idually by host-derived symbiosomal membranes and are housed within specialized host bacteriocyte cells. The transport capabilities of the symbiosomal membrane remain unknown. Here, we identify a transport system that mediates a crucial step in this metabolic complementarity: a transporter capable of transporting nonessential amino acids across the symbiosomal membrane of the pea aphid Acyrthosiphon pisum .
Publisher: American Physiological Society
Date: 02-2021
DOI: 10.1152/AJPLUNG.00137.2020
Abstract: Cystic fibrosis (CF) arises from mutations in the CF transmembrane conductance regulator ( CFTR) gene, resulting in progressive and life-limiting respiratory disease. R751L is a rare CFTR mutation that is poorly characterized. Our aims were to describe the clinical and molecular phenotypes associated with R751L. Relevant clinical data were collected from three heterozygote in iduals harboring R751L (2 patients with G551D/R751L and 1 with F508del/R751L). Assessment of R751L-CFTR function was made in primary human bronchial epithelial cultures (HBEs) and Xenopus oocytes. Molecular properties of R751L-CFTR were investigated in the presence of known CFTR modulators. Although sweat chloride was elevated in all three patients, the clinical phenotype associated with R751L was mild. Chloride secretion in F508del/R751L HBEs was reduced compared with non-CF HBEs and associated with a reduction in sodium absorption by the epithelial sodium channel (ENaC). However, R751L-CFTR function in Xenopus oocytes, together with folding and cell surface transport of R751L-CFTR, was not different from wild-type CFTR. Overall, R751L-CFTR was associated with reduced sodium chloride absorption but had functional properties similar to wild-type CFTR. This is the first report of R751L-CFTR that combines clinical phenotype with characterization of functional and biological properties of the mutant channel. Our work will build upon existing knowledge of mutations within this region of CFTR and, importantly, inform approaches for clinical management. Elevated sweat chloride and reduced chloride secretion in HBEs may be due to alternative non-CFTR factors, which require further investigation.
Publisher: American Physiological Society
Date: 10-2010
DOI: 10.1152/AJPCELL.00184.2010
Abstract: The δ-subunit of the epithelial Na + channel (ENaC) is expressed in neurons of the human and monkey central nervous system and forms voltage-independent, amiloride-sensitive Na + channels when expressed in heterologous systems. It has been proposed that δ-ENaC could affect neuronal excitability and participate in the transduction of ischemic signals during hypoxia or inflammation. The regulation of δ-ENaC activity is poorly understood. ENaC channels in kidney epithelial cells are regulated by the serum- and glucocorticoid-induced kinase 1 (SGK1). Recently, a new isoform of this kinase (SGK1.1) has been described in the central nervous system. Here we show that δ-ENaC isoforms and SGK1.1 are coexpressed in pyramidal neurons of the human and monkey ( Macaca fascicularis ) cerebral cortex. Coexpression of δβγ-ENaC and SGK1.1 in Xenopus oocytes increases amiloride-sensitive current and channel plasma membrane abundance. The kinase also exerts its effect when δ-subunits are expressed alone, indicating that the process is not dependent on accessory subunits or the presence of PY motifs in the channel. Furthermore, SGK1.1 action depends on its enzymatic activity and binding to phosphatidylinositol( 4 , 5 )-bisphosphate. Physiological or pharmacological activation of phospholipase C abrogates SGK1.1 interaction with the plasma membrane and modulation of δ-ENaC. Our data support a physiological role for SGK1.1 in the regulation of δ-ENaC through a pathway that differs from the classical one and suggest that the kinase could serve as an integrator of different signaling pathways converging on the channel.
Location: Germany
Location: United Kingdom of Great Britain and Northern Ireland
No related grants have been discovered for Mike Althaus.