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Paul Kaae posted an update 1 week, 5 days ago
It is proved that AS supplementation can enhance innate immunity and change several relevant immune factors and cells of healthy mice without affecting growth performance.
Literature on trial of labor after cesarean section (TOLAC) in women with isthmoceles is scarce because of complications associated with the procedure. This study investigated TOLAC’s safety and feasibility in patients with isthmoceles.
The study group comprised 34 pregnant women with isthmoceles who vaginally delivered. The control group comprised 102 pregnant women without isthmoceles who vaginally delivered during the same period. Scar diverticula were measured using color Doppler ultrasonography; between-group delivery outcomes were compared.
Of the study group patients, 27/34 had isthmoceles diagnosed by ultrasound before pregnancy. Nineteen (70.37%) of these patients had mild defects and eight (29.63%) had moderate defects. The scar diverticula’s mean length, depth, and width were 1.05 ± 0.62, 0.54 ± 0.28, and 1.20 ± 0.70 cm, respectively. The residual muscle layer’s mean thickness was 0.27 ± 0.07 cm. The mean diverticulum depth/residual muscular thickness ratio was 2.39 ± 2.58. The duration of the first stage of labor was significantly shorter and the neonatal weight was significantly lower in the study group than control group.
Successful vaginal delivery is possible for women with mild and moderate isthmoceles. Further large-scale studies are needed to improve TOLAC’s safety in pregnant women with isthmoceles.
Successful vaginal delivery is possible for women with mild and moderate isthmoceles. Further large-scale studies are needed to improve TOLAC’s safety in pregnant women with isthmoceles.The amount of sequencing data is growing at a fast pace due to a rapid revolution in sequencing technologies. Quality scores, which indicate the reliability of each of the called nucleotides, take a significant portion of the sequencing data. In addition, quality scores are more challenging to compress than nucleotides, and they are often noisy. Hence, a natural solution to further decrease the size of the sequencing data is to apply lossy compression to the quality scores. Lossy compression may result in a loss in precision, however, it has been shown that when operating at some specific rates, lossy compression can achieve performance on variant calling similar to that achieved with the losslessly compressed data (i.e. the original data). We propose Coding with Random Orthogonal Matrices for quality scores (CROMqs), the first lossy compressor designed for the quality scores with the “infinitesimal successive refinability” property. With this property, the encoder needs to compress the data only once, at a high rate, while the decoder can decompress it iteratively. The decoder can reconstruct the set of quality scores at each step with reduced distortion each time. This characteristic is specifically useful in sequencing data compression, since the encoder does not generally know what the most appropriate rate of compression is, e.g. for not degrading variant calling accuracy. CROMqs avoids the need of having to compress the data at multiple rates, hence incurring time savings. In addition to this property, we show that CROMqs obtains a comparable rate-distortion performance to the state-of-the-art lossy compressors. selleck chemicals Moreover, we also show that it achieves a comparable performance on variant calling to that of the lossless compressed data while achieving more than 50% reduction in size.Gleason score (GS) is a powerful prognostic factor in prostate cancer (PCa). A GS-7 tumor typically has the primary Gleason (architectural) pattern and secondary prevalent one being graded with 3 and 4 (or 4 and 3), respectively. Due to the well-known intratumoral multifocal occurrence of different patterns, a biological sample from a GS-7 tumor used in a molecular experiment will be uncertain regarding the actually represented pattern if no special attention is given to specimen preparation. In this study, by an integrative analysis of several published gene expression datasets, one of which is the profiling of the paired GP-3 (Gleason pattern 3) and GP-4 (Gleason pattern 4) specimens of 13 GS-7 tumors, we demonstrate that such an uncertainty can be frequently observed in the published data. More specifically, our results suggest that the GS-7 specimens used to generate the frequently-cited The Cancer Genome Atlas (TCGA) data and the Gene Expression Omnibus (GEO) dataset GSE21032 which largely are individual GP-3 or GP-4 specimens rather than the “intermediate” specimens of GP-3 and GP-4. This indicates a pitfall in the existing molecular research of prostate tumors relevant to GS and in GS-related molecular biomarker identification using the previously documented data.
To study the characteristics of the intestinal flora in patients with diabetic peripheral neuropathy (DPN) and analyze the association between the intestinal flora and clinical indicators.
We classified 80 subjects into three groups patients with DPN (n = 45), patients type 2 diabetes without DPN (n = 21), and healthy controls (n = 14). The intestinal flora composition was compared among the three groups, and the correlation between the intestinal flora and clinical indicators was analyzed.
At the phylum level, the richness of Firmicutes and Actinobacteria was elevated in the DN group, and that of Bacteroidetes was decreased. At the genus level, the richness of
and
was significantly decreased in the DPN group, whereas that of
–
,
,
,
, and
group was increased. The homeostasis model assessment insulin resistance index was positively correlated with
richness. Glycine ursodeoxycholic acid was positively correlated with
group and
richness. Tauroursodeoxycholic acid was positively correlated with
group and
richness.
There was obvious intestinal microbiota disorder in patients with DPN, which may be related to insulin resistance. These changes may have important roles in the development of DPN.
There was obvious intestinal microbiota disorder in patients with DPN, which may be related to insulin resistance. These changes may have important roles in the development of DPN.