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2. Accuracy of Hospital Monitor Respiratory Rates Compared to Manual Counts in Children

Author

Parlar-Chun, Raymond, Area, Makenna, Marshburn, Ann, Lafferty-Prather, Meaghan, Saleh, Zeina, and Hsu, Jean

Subjects
Respiration -- Evaluation, Patient monitoring -- Methods, Pediatric research, Health
Abstract

Purpose: Respiratory rates are an important vital sign for the hospitalized patient and are often counted by monitors. We assessed the accuracy of monitor readings when compared to manual counts stratified by patient age and diagnosis. Design and Methods: Hospitalized children aged 0 to 17 years placed on monitors were eligible. Respiratory rates were stratified by age and diagnosis-respiratory versus non-respiratory. Monitor respiratory rates were recorded every 3 seconds for duration of one minute. Concurrent manual counts were performed at 5, 10, 15, 30, and 60 seconds. Bland-Altman method was used to assess agreement between manual 60 second counts and the monitored respiratory rate. Results: Enrollment included 181 patients of which the majority (n = 93, 51%), were less than age 12 months, and 114 (63%) had non-respiratory diagnoses. The mean difference of the following interval manual counts compared to 60-second manual counts were +4.3 (overestimation) breaths with 6-second measurements, +3 breaths for 10 seconds, +1.6 breaths for 15 seconds, +1.3 breaths for 20 seconds, and +0.6 breaths for 30-second measurements. The mean difference of hospital monitors was -7.2 (underestimation) breaths. Monitor counts had increasing underestimation with increasing respiratory rates. There was significant underestimation of monitor respiratory rates compared to 60-second manual counts in infants less than age 6 months. There was no significant difference between respiratory and non-respiratory diagnoses. Conelusion: Hospital monitors underestimate respiratory rates compared to manual counts. Applieation to Praetiee: Clinicians should exercise caution in using monitor-generated respiratory rates to assess patient status, particularly in infants and those expected to have high respiratory rates. We found under-estimation of respiratory rates in these patients, which may lead to falsely low clinical screening and severity scores. Key Words: Hospital monitors, respiratory rates, manual counts, hospital pediatrics., Respiratory rates are an essential vital sign in hospitalized children. Common reasons for pediatric hospitalizations, such as bronchiolitis, pneumonia, and sepsis, require accurate assessments of respiratory rates, and many pediatric [...]

Published
2023

3. Intranasal sensitization model of alopecia areata using pertussis toxin as adjuvant.

Author

Yuying Liu, Freeborn, Jasmin, Okeugo, Beanna, Armbrister, Shabba A., Saleh, Zeina M., Alvarez, Ana Beatriz Fadhel, Hoang, Thomas K., Park, Evelyn S., Lindsey, John William, Rapini, Ronald P., Glazer, Steven, Rubin, Keith, and Rhoads, Jon Marc

Subjects
PERTUSSIS toxin, BORDETELLA pertussis, INTRANASAL administration, B cells, CELLULAR immunity, ALOPECIA areata
Abstract

Background: Nasopharyngeal Bordetella pertussis (BP) colonization is common, with about 5% of individuals having PCR evidence of subclinical BP infection on nasal swab, even in countries with high vaccination rates. BP secretes pertussis toxin (PTx). PTx is an adjuvant commonly used to induce autoimmunity in multiple animal models of human disease. Colocalization of PTx and myelin from myelinated nerves in the nasopharynx may lead to host sensitization to myelin with subsequent autoimmune pathology. Methods: C57BL/6J female adult mice were given varied doses and schedules of intranasal PTx, MOG35-55 antigen, or controls to test whether intranasal administration of PTx and myelin oligodendrocyte peptide (MOG35-55) could induce experimental autoimmune encephalomyelitis (EAE) in mice. While we observed systemic cell-mediated immunity against MOG35-55, we did not observe EAE. Unexpectedly, many mice developed alopecia. We systematically investigated this finding. Results: Patchy alopecia developed in 36.4% of mice with the optimized protocol. Pathology consistent with alopecia areata was confirmed histologically by documenting concomitant reduced anagen phase and increased telogen phase hair follicles (HFs) in biopsies from patches of hair loss in mice with alopecia. We also found reduced CD200 staining and increased CD3+T cells surrounding the HFs of mice with alopecia compared to the mice without alopecia, indicating HF Immune Privilege (HFIP) collapse. Systemic immune responses were also found, with increased proportions of activated T cells and B cells, as well as MHCII+ dendritic cells in peripheral blood and/or splenocytes. Finally, in mice initially exposed to intranasal MOG35-55 and PTx in combination, but not to either agent alone, splenocytes were shown to proliferate after in vitro stimulation by MOG35-55. Consistent with prior investigations, PTx exhibited a dose-response effect on immune cell induction and phenotype, with the lowest PTx dose failing to induce autoimmunity, the highest PTx dose suppressing autoimmunity, and intermediate doses optimizing autoimmunity. Conclusions: We propose that this is the first report of an autoimmune disease in an animal model triggered by colocalization of intranasal PTx and autoantigen. This model parallels a natural exposure and potential intranasal sensitization-topathology paradigm and supports the plausibility that nasopharyngeal subclinical BP colonization is a cause of alopecia areata. [ABSTRACT FROM AUTHOR]

Published
2024
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4. The burden of laboratory-confirmed influenza infection in Lebanon between 2008 and 2016: a single tertiary care center experience

Author

Assaf-Casals, Aia, Saleh, Zeina, Khafaja, Sarah, Fayad, Danielle, Ezzeddine, Hady, Saleh, Mohammad, Chamseddine, Sarah, Sayegh, Rouba, Sharara, Sima L., Chmaisse, Ahmad, Kanj, Souha S., Kanafani, Zeina, Hanna-Wakim, Rima, Araj, George F., Mahfouz, Rami, Saito, Reiko, Suzuki, Hiroshi, Zaraket, Hassan, and Dbaibo, Ghassan S.

Published
2020
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8. Columnar Metaplasia of the Esophagus Presenting as Iron Deficiency Anemia in Children with Neurologic Impairment or Congenital Esophageal Atresia.

Author

Van Arsdall, Melissa R., Nair, Supriya, Moye, Lindsay M., Nguyen, Trinh T., Saleh, Zeina M., and Rhoads, J. Marc

Subjects
ESOPHAGEAL atresia, IRON deficiency anemia, METAPLASIA, BARRETT'S esophagus, ESOPHAGUS, PATHOLOGY
Abstract

Objective: Rare coexistence of disease or pathology Background: Columnar metaplasia of the lower esophagus includes both gastric and intestinal metaplasia. Children with severe neurologic impairment and congenital esophageal atresia often have gastroesophageal reflux disease, which can lead to Barrett's esophagus, a form of lower esophageal columnar metaplasia and precursor to esophageal adenocarcinoma, with some, but not all, guidelines specifically requiring the presence of intestinal metaplasia for diagnosis. This case series illustrates how iron deficiency anemia may be the primary symptom of esophageal columnar metaplasia in such children and how upper endoscopy is essential in their initial and ongoing evaluation. Case Reports: We review 5 cases of columnar metaplasia of the lower esophagus in children, 3 with severe neurologic impairment and 2 with esophageal atresia. Each child presented with marked iron deficiency anemia and minimal-to-no gastrointestinal symptoms. Conclusions: We conclude that columnar metaplasia of the esophagus may present with iron deficiency anemia in children with neurologic impairment or congenital esophageal atresia, even if without overt gastrointestinal symptoms. Accordingly, we propose that early endoscopic evaluation should be considered in this specific patient population. Based on our literature review, we also emphasize the need for guidelines on the endoscopic surveillance of such children with any type of columnar metaplasia of the lower esophagus, given the associated risk of malignant transformation. [ABSTRACT FROM AUTHOR]

Published
2022
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10. Intranasal sensitization model of alopecia areata using pertussis toxin as adjuvant.

Author

Liu Y, Freeborn J, Okeugo B, Armbrister SA, Saleh ZM, Fadhel Alvarez AB, Hoang TK, Park ES, Lindsey JW, Rapini RP, Glazer S, Rubin K, and Rhoads JM

Subjects
Animals, Mice, Female, Peptide Fragments immunology, Peptide Fragments administration & dosage, Bordetella pertussis immunology, Whooping Cough immunology, Pertussis Toxin immunology, Pertussis Toxin administration & dosage, Administration, Intranasal, Disease Models, Animal, Alopecia Areata immunology, Encephalomyelitis, Autoimmune, Experimental immunology, Adjuvants, Immunologic administration & dosage, Mice, Inbred C57BL, Myelin-Oligodendrocyte Glycoprotein immunology, Myelin-Oligodendrocyte Glycoprotein administration & dosage
Abstract

Background: Nasopharyngeal Bordetella pertussis (BP) colonization is common, with about 5% of individuals having PCR evidence of subclinical BP infection on nasal swab, even in countries with high vaccination rates. BP secretes pertussis toxin (PTx). PTx is an adjuvant commonly used to induce autoimmunity in multiple animal models of human disease. Colocalization of PTx and myelin from myelinated nerves in the nasopharynx may lead to host sensitization to myelin with subsequent autoimmune pathology., Methods: C57BL/6J female adult mice were given varied doses and schedules of intranasal PTx, MOG 35-55 antigen, or controls to test whether intranasal administration of PTx and myelin oligodendrocyte peptide (MOG 35-55 ) could induce experimental autoimmune encephalomyelitis (EAE) in mice. While we observed systemic cell-mediated immunity against MOG 35-55 , we did not observe EAE. Unexpectedly, many mice developed alopecia. We systematically investigated this finding., Results: Patchy alopecia developed in 36.4% of mice with the optimized protocol. Pathology consistent with alopecia areata was confirmed histologically by documenting concomitant reduced anagen phase and increased telogen phase hair follicles (HFs) in biopsies from patches of hair loss in mice with alopecia. We also found reduced CD200 staining and increased CD3 + T cells surrounding the HFs of mice with alopecia compared to the mice without alopecia, indicating HF Immune Privilege (HFIP) collapse. Systemic immune responses were also found, with increased proportions of activated T cells and B cells, as well as MHCII + dendritic cells in peripheral blood and/or splenocytes. Finally, in mice initially exposed to intranasal MOG 35-55 and PTx in combination, but not to either agent alone, splenocytes were shown to proliferate after in vitro stimulation by MOG 35-55. Consistent with prior investigations, PTx exhibited a dose-response effect on immune cell induction and phenotype, with the lowest PTx dose failing to induce autoimmunity, the highest PTx dose suppressing autoimmunity, and intermediate doses optimizing autoimmunity., Conclusions: We propose that this is the first report of an autoimmune disease in an animal model triggered by colocalization of intranasal PTx and autoantigen. This model parallels a natural exposure and potential intranasal sensitization-to-pathology paradigm and supports the plausibility that nasopharyngeal subclinical BP colonization is a cause of alopecia areata., Competing Interests: KR and SG are employed by ILiAD Biotechnologies LLC, which is developing a vaccine for the prevention of Bordetella pertussis infection. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest. Author YL declared that they were an editorial board member of Frontiers, at the time of submission. This had no impact on the peer review process and the final decision. The authors declare that this study received funding from ILiAD Biotechnologies LLC (P00427002 to JR). The funder had the following involvement in the study: the study design and the writing of this article (review and edit)., (Copyright © 2024 Liu, Freeborn, Okeugo, Armbrister, Saleh, Fadhel Alvarez, Hoang, Park, Lindsey, Rapini, Glazer, Rubin and Rhoads.)

Published
2024
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11. Probiotic-derived ecto-5'-nucleotidase produces anti-inflammatory adenosine metabolites in Treg-deficient scurfy mice.

Author

Liu Y, Armbrister SA, Okeugo B, Mills TW, Daniel RC, Oh JH, Pijkeren JP, Park ES, Saleh ZM, Lahiri S, Roos S, and Rhoads JM

Abstract

Probiotic Limosilactobacillus reuteri DSM 17938 (DSM 17938) prolonges the survival of Treg-deficient scurfy (SF) mice and reduces multiorgan inflammation by a process requiring adenosine receptor 2A (A 2A ) on T cells. We hypothesized that L. reuteri -derived ecto-5'-nucleotidase (ecto-5'NT) activity acts to generate adenosine, which may be a central mediator for L. reuteri protection in SF mice. We evaluated DSM 17938-5'NT activity and the associated adenosine and inosine levels in plasma, gut and liver of SF mice. We examined orally fed DSM 17938, DSM 17938Δ5NT (with a deleted 5'NT gene), and DSM 32846 (BG-R46) (a naturally selected strain derived from DSM 17938). Results showed that DSM 17938 and BG-R46 produced adenosine while "exhausting" AMP, whereas DSM 17938∆5NT did not generate adenosine in culture. Plasma 5'NT activity was increased by DSM 17938 or BG-R46, but not by DSM 17938Δ5NT in SF mice. BG-R46 increased both adenosine and inosine levels in the cecum of SF mice. DSM 17938 increased adenosine levels, whereas BG-R46 increased inosine levels in the liver. DSM 17938Δ5NT did not significantly change the levels of adenosine or inosine in the GI tract or the liver of SF mice. Although regulatory CD73 + CD8 + T cells were decreased in spleen and blood of SF mice, these regulatory T cells could be increased by orally feeding DSM 17938 or BG-R46, but not DSM 17938Δ5NT. In conclusion, probiotic-5'NT may be a central mediator of DSM 17938 protection against autoimmunity. Optimal 5'NT activity from various probiotic strains could be beneficial in treating Treg-associated immune disorders in humans.

Published
2023
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12. Applications of Tissue Engineering in Joint Arthroplasty: Current Concepts Update.

Author

Zeineddine HA, Frush TJ, Saleh ZM, El-Othmani MM, and Saleh KJ

Subjects
Humans, Orthopedics trends, Arthroplasty instrumentation, Arthroplasty methods, Arthroplasty trends, Cartilage Diseases surgery, Tissue Engineering methods, Tissue Engineering trends
Abstract

Research in tissue engineering has undoubtedly achieved significant milestones in recent years. Although it is being applied in several disciplines, tissue engineering's application is particularly advanced in orthopedic surgery and in degenerative joint diseases. The literature is full of remarkable findings and trials using tissue engineering in articular cartilage disease. With the vast and expanding knowledge, and with the variety of techniques available at hand, the authors aimed to review the current concepts and advances in the use of cell sources in articular cartilage tissue engineering., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published
2017
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