44 research outputs found
Alteration of sarcoplasmic reticulum Ca<sup>2+</sup> ATPase expression in lower limb ischemia caused by atherosclerosis obliterans
Atherosclerosis is a disease caused by a build-up of fatty plaques and cholesterol in the arteries. The lumen of the vessels is obliterated resulting in restricted blood supply to tissues. In ischemic conditions, the cytosolic Ca2+ level of skeletal muscle may increase, indicating the alteration of Ca2+ removal mechanisms. Ca2+ is transported from cytosol into the sarcoplasmic reticulum by Ca2+ ATPase (SERCA), with its 1a isoform expressed in adult, while its 1b isoform in neonatal and regenerating fast-twitch skeletal muscle. To investigate the role of these isoforms in ischemic skeletal muscle, biopsies from musculus biceps femoris of patients who underwent amputation due to atherosclerosis were examined. Samples were removed from the visibly healthy and hypoxia-affected tissue. Significantly increased SERCA1a expression was detected under the ischemic conditions (246 ± 69%; p  0.05), whereas SERCA2a did not change. In addition, in primary cultures derived from hypoxia-affected tissue, the diameter and fusion index of myotubes were significantly increased (30 ± 1.6 µm vs. 41 ± 2.4 µm and 31 ± 4% vs. 45 ± 3%; p < 0.05). We propose that the increased SERCA1a expression indicates the existence and location of compensating mechanisms in ischemic muscle
Molecular structure and developmental expression of zebrafish atp2a genes
[[abstract]]We isolated two atp2a genes, atp2a1 and atp2a2a, from embryonic zebrafish. Amino acid sequences deduced from zebrafish atp2a genes are aligned with orthologue proteins from other species, the results showed that they share high percentage of identities (82%–94%) and acidic pIs (5.03–5.33). Whole mount in situ hybridization experiments showed that atp2a1 and atp2a2a are maternal inherited genes which can be detected at 1-cell stage embryos and express in the entire animal pole from 6 hours post-fertilization (hpf) to 12 hpf. At the later stages (48–96 hpf), expression of atp2a1 was restricted in head and trunk muscles as well as in some neurons. In contrast to the strongly expression of atp2a1 in head muscle, expression of atp2a2a was detected in head muscle in a fainter manner. In addition, transcripts of atp2a2a were observed in the developing heart during early cardiogenesis. The present studies not only help us to comparatively analyze atp2a genes across species, but also provide useful information about expressions during early embryogenesis that will help in further investigations of functional studies of Atp2a in the future.[[incitationindex]]SCI[[booktype]]紙
Kinetics of 1,6-hydrogen migration in alkyl radical reaction class
The kinetics of the 1,6-intramolecular hydrogen migration in the alkyl
radical reaction class has been studied using the reaction class transition state theory
(RC-TST) combined with the linear energy relationship (LER) and the barrier height
grouping (BHG) approach. The RC-TST/LER, where only reaction energy is needed,
and RC-TST/BHG, where no other information is needed, are found to be promising
methods for predicting rate constants for any reaction in the 1,6-intramolecular H
migration in alkyl radicals reaction class. Direct comparison with available experimental
data indicates that the RC-TST/LER, where only reaction energy is needed, can
predict rate constants for any reaction in this reaction class with satisfactory accuracy
Silencing SERCA1b in a few fibers stimulates growth in the entire regenerating soleus muscle
The neonatal isoform of the sarcoplasmic/endoplasmic
reticulum Ca2+ ATPase 1 (SERCA1b) is a dominant
Ca2+ pump in the young Wbers of regenerating muscle.
In vivo transfection of about 1% of the Wbers with
SERCA1b RNAi plasmid resulted in no apparent change in
the transfected Wbers, but enhanced the increase of fresh
weight and Wber size in the whole regenerating rat soleus
muscle, until the normal size was reached. Co-transfection
of calcineurin inhibitor cain/cabin-1 with SERCA1b RNAi
was suYcient to cut down the widespread growth stimulation,
but the subsequent transfection of cain into the
SERCA1b RNAi transfected muscle did not inhibit muscle
growth. The SERCA1b RNAi preferably upregulated the expression of the NFAT reporter lacZ compared to controls
when co-transfected into the Wbers. Notably, perimuscular
injection of interleukin-4 (IL-4) antibody but not that of an
unrelevant antibody completely abolished the growth-promoting
eVect of SERCA1b RNAi. This indicates that
silencing SERCA1b in a few Wbers stimulates the calcineurin-
NFAT-IL-4 pathway and Wber growth in the whole
regenerating soleus. These results suggest the presence of
an autocrine–paracrine coordination of growing muscle
Wbers, and put forward a new method to stimulate skeletal
muscle regeneration
Opioid receptor activity and analgesic potency of DPDPE peptide analogues containing a xylene bridge.
d-Pen2,d-Pen5 enkephalin (DPDPE) is one of the most selective synthetic peptide agonists targeting the δ-opioid receptor. Three cyclic analogues of DPDPE containing a xylene bridge in place of disulfide bond have been synthesized and fully characterized as opioid receptors agonists. The in vitro activity was investigated showing a good affinity of 7a-c for μ- and δ-receptors. In vivo biological assays revealed that 7b is the most potent analogue with the ability to maintain high level of analgesia from 15 to 60 min following intracerebroventricular (i.c.v.) administration, whereas DPDPE was slightly active until 45 min. Compound 7b induced long lasting analgesia also after subcutaneous administration, whereas DPDPE was inactive