Badr AlSaleem scite author profile

Badr AlSaleem

4Publications

48Citation Statements Received

61Citation Statements Given

How they've been cited

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130

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King Fahd Medical City

Publications

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Diagnostic delay of pediatric inflammatory bowel disease in Saudi Arabia

Mouzan¹,

AlSaleem²,

Hasosah³

et al. 2019

Saudi J Gastroenterol

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Background/Aim: Delay in the diagnosis of inflammatory bowel disease (IBD) is associated with complications. Our aim was to describe the pattern and risk factors associated with delay in the diagnosis of IBD in Saudi children. Patients and Methods: This was a multicenter study with a retrospective/prospective design. Data on diagnostic delay in children with Crohn's disease (CD) and ulcerative colitis (UC) were retrieved from physician's notes. Multivariate regression analysis was used to assess the risk factors associated with long delay in diagnosis. Results: There were 240 and 183 Saudi children with CD and UC, respectively. The median delays in diagnosis were 8 and 5 months in CD and UC, respectively, significantly longer in children with CD than UC ( P < 0.001). Long diagnostic delays (>75 th percentile) were 24 and 8.8 months for CD and UC, respectively. Ileal location was a significant risk factor in CD and the age of onset above 10 years was protective in UC. Conclusions: Long diagnostic delay in IBD was mainly due to the longer delay in gastroenterologist consultation. Review of the referral system is needed to focus on measures to reduce long delays in diagnosis. The ileal location as a risk factor in CD and age older than 10 years as protective in UC should help recognition and early referral.

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Fungal Dysbiosis in Children with Celiac Disease

et al. 2021

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Viral dysbiosis in children with new-onset celiac disease

et al. 2022

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Viruses are common components of the intestinal microbiome, modulating host bacterial metabolism and interacting with the immune system, with a possible role in the pathogenesis of immune-mediated diseases such as celiac disease (CeD). The objective of this study was to characterize the virome profile in children with new-onset CeD. We used metagenomic analysis of viral DNA in mucosal and fecal samples from children with CeD and controls and performed sequencing using the Nextera XT library preparation kit. Abundance log2 fold changes were calculated using differential expression and linear discriminant effect size. Shannon alpha and Bray–Curtis beta diversity were determined. A total of 40 children with CeD and 39 controls were included. We found viral dysbiosis in both fecal and mucosal samples. Examples of significantly more abundant species in fecal samples of children with CeD included Human polyomavirus 2, Enterobacteria phage mEpX1, and Enterobacteria phage mEpX2; whereas less abundant species included Lactococcus phages ul36 and Streptococcus phage Abc2. In mucosal samples however, no species were significantly associated with CeD. Shannon alpha diversity was not significantly different between CeD and non-CeD groups and Bray–Curtis beta diversity showed no significant separation between CeD and non-CeD samples in either mucosal or stool samples, whereas separation was clear in all samples. We identified significant viral dysbiosis in children with CeD, suggesting a potential role in the pathogenesis of CeD indicating the need for further studies.

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Use of oral iron in managing iron deficiency anemia in children with intestinal failure

AlSaleem

Albanyan

Alamer

et al. 2021

Journal of King Saud University - Science

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Badr AlSaleem

Diagnostic delay of pediatric inflammatory bowel disease in Saudi Arabia

Fungal Dysbiosis in Children with Celiac Disease

Viral dysbiosis in children with new-onset celiac disease

Use of oral iron in managing iron deficiency anemia in children with intestinal failure

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