St Pierre, T. G., Y. Aydinok, A. El-Beshlawy, S. Bayraktaroglu, A. Ibrahim, M. HAMDY, W. Pang, S. Khorshid, S. Bangma, and M. House, "5613049 THE DIAGNOSTIC ACCURACY AND REPEATABILITY OF AN ARTIFICIAL INTELLIGENCE BASED SYSTEM TO OBTAIN AUTOMATED LIVER IRON CONCENTRATION MEASUREMENTS USING MAGNETIC RESONANCE IMAGING.", Blood Advances, vol. volume 7, issue issue 4, pp. 611-619, 2023.
Vitrano, A., K. M. Musallam, A. Meloni, M. Karimi, S. Daar, P. Ricchi, S. Costantini, E. Vlachaki, V. Di Marco, A. El-Beshlawy, et al., "Development of a Thalassemia International Prognostic Scoring System (TIPSS).", Blood cells, molecules & diseases, vol. 99, pp. 102710, 2023. Abstract

A prognostic scoring system that can differentiate β-thalassemia patients based on mortality risk is lacking. We analysed data from 3145 β-thalassemia patients followed through a retrospective cohort design for the outcome of death. An a priori list of prognostic variables was collected. β Coefficients from a multivariate cox regression model were used from a development dataset (n = 2516) to construct a formula for a Thalassemia International Prognostic Scoring System (TIPSS) which was subsequently applied to a validation dataset (n = 629). The median duration of observation was 10.0 years. The TIPSS score formula was constructed as exp (1.4 × heart disease + 0.9 × liver disease + 0.9 × diabetes + 0.9 × sepsis + 0.6 × alanine aminotransferase ≥42 IU/L + 0.6 × hemoglobin ≤9 g/dL + 0.4 × serum ferritin ≥1850 ng/mL). TIPSS score thresholds of greatest differentiation were assigned as <2.0 (low-risk), 2.0 to <5.0 (intermediate-risk), and ≥5.0 (high-risk). The TIPSS score was a good predictor for the outcome of death in the validation dataset (AUC: 0.722, 95%CI: 0.641-0.804) and survival was significantly different between patients in the three risk categories (P < 0.001). Compared to low-risk patients, the hazard ratio for death was 2.778 (95%CI: 1.335-5.780) in patients with intermediate-risk and 6.431 (95%CI: 3.151-13.128) in patients with high-risk. This study provides a novel tool to support mortality risk categorization for patients with β-thalassemia that could help management and research decisions.

yomna said mohamed, A. M. E. - Beshlawy, H. A. Sabry, D. S. Sabry, and M. kamal Mohamed, "Relation Between Salivary Immunoglobulins Levels and Dental Caries in Egyptian Children with Gaucher Disease", Egyptian Dental Journal, vol. Volume 70, issue Issue 2 , 2024.
Hassan, S., G. Baselli, L. Mollica, R. L. Rossi, H. Chand, A. El-Beshlawy, M. Elalfy, V. Ramanan, P. Eshghi, M. Karimi, et al., "Predicting inhibitor development using a random peptide phage-display library approach in the SIPPET cohort.", Blood advances, vol. 8, issue 11, pp. 2880-2889, 2024. Abstract

Inhibitor development is the most severe complication of hemophilia A (HA) care and is associated with increased morbidity and mortality. This study aimed to use a novel immunoglobulin G epitope mapping method to explore the factor VIII (FVIII)-specific epitope profile in the SIPPET cohort population and to develop an epitope mapping-based inhibitor prediction model. The population consisted of 122 previously untreated patients with severe HA who were followed up for 50 days of exposure to FVIII or 3 years, whichever occurred first. Sampling was performed before FVIII treatment and at the end of the follow-up. The outcome was inhibitor development. The FVIII epitope repertoire was assessed by means of a novel random peptide phage-display assay. A least absolute shrinkage and selection operator (LASSO) regression model and a random forest model were fitted on posttreatment sample data and validated in pretreatment sample data. The predictive performance of these models was assessed by the C-statistic and a calibration plot. We identified 27 775 peptides putatively directed against FVIII, which were used as input for the statistical models. The C-statistic of the LASSO and random forest models were good at 0.78 (95% confidence interval [CI], 0.69-0.86) and 0.80 (95% CI, 0.72-0.89). Model calibration of both models was moderately good. Two statistical models, developed on data from a novel random peptide phage display assay, were used to predict inhibitor development before exposure to exogenous FVIII. These models can be used to set up diagnostic tests that predict the risk of inhibitor development before starting treatment with FVIII.

HAMDY, M. O. N. A., A. El-Beshlawy, M. P. A. Veríssimo, J. Kanter, B. Inusa, S. Williams, D. Lee, N. T. Temin, C. Fradette, F. Tricta, et al., "Deferiprone versus deferoxamine for transfusional iron overload in sickle cell disease and other anemias: Pediatric subgroup analysis of the randomized, open-label FIRST study.", Pediatric blood & cancer, vol. 71, issue 1, pp. e30711, 2024. Abstract

BACKGROUND: Children with sickle cell disease (SCD) who are chronically transfused often, require iron chelation therapy. There are limited data that allow for comparison of the efficacy and safety of the iron chelator deferiprone versus deferoxamine in children with SCD.

METHODS: This post hoc analysis of the phase 3b/4, randomized, open-label FIRST (Ferriprox in Patients with IRon Overload in Sickle Cell Disease Trial) study (NCT02041299) included patients 17 years and younger with SCD or other anemias receiving deferiprone or deferoxamine.

RESULTS: Overall, 142 patients were evaluated; mean ages were 10.5 and 11.7 years in the deferiprone and deferoxamine groups, respectively. At 12 months: mean change from baseline in liver iron concentration was -3.3 mg/g dry weight (dw) with deferiprone and -3.4 mg/g dw with deferoxamine (p = .8216); relative mean change (coefficient of variation %) in log cardiac T2* magnetic resonance imaging was 1.02 (21.8%) with deferiprone and 0.95 (19.5%) with deferoxamine (p = .0717); and the mean (standard error) change in serum ferritin levels was -133.0 (200.3) μg/L with deferiprone and -467.1 (244.1) μg/L with deferoxamine (p = .2924). The most common deferiprone-related adverse events (AEs) were upper abdominal pain (20.2%), vomiting (13.8%), pyrexia (9.6%), decreased neutrophil count (9.6%), increased alanine aminotransferase (ALT; 9.6%), and increased aspartate aminotransferase (AST; 9.6%). All cases of increased ALT, increased AST, and neutropenia resolved, most without intervention.

CONCLUSIONS: This post hoc analysis of pediatric patients from FIRST corroborated previous findings in adults that deferiprone is comparable to deferoxamine in reducing iron overload. No new safety concerns were observed. Deferiprone is an oral chelation option that could improve adherence and outcomes in children.

El-Beshlawy, A., H. Dewedar, S. Hindawi, S. Alkindi, A. A. Tantawy, M. A. Yassin, and A. T. Taher, "Management of transfusion-dependent β-thalassemia (TDT): Expert insights and practical overview from the Middle East.", Blood reviews, vol. 63, pp. 101138, 2024. Abstract

β-Thalassemia is one of the most common monogenetic diseases worldwide, with a particularly high prevalence in the Middle East region. As such, we have developed long-standing experience with disease management and devising solutions to address challenges attributed to resource limitations. The region has also participated in the majority of clinical trials and development programs of iron chelators and more novel ineffective erythropoiesis-targeted therapy. In this review, we provide a practical overview of management for patients with transfusion-dependent β-thalassemia, primarily driven by such experiences, with the aim of transferring knowledge to colleagues in other regions facing similar challenges.

Musallam, K. M., M. D. Cappellini, S. Daar, A. El-Beshlawy, and A. T. Taher, "Magnitude of cumulative iron overload correlates with the severity of anemia in untreated non-transfusion-dependent β-thalassemia.", Annals of hematology, vol. 102, issue 2, pp. 467-469, 2023.
Elalfy, M. S., M. O. N. A. HAMDY, A. El-Beshlawy, F. S. Ebeid, M. Badr, J. Kanter, B. Inusa, A. A. M. Adly, S. Williams, Y. Kilinc, et al., "Deferiprone for transfusional iron overload in sickle cell disease and other anemias: open-label study of up to 3 years.", Blood advances, vol. 7, issue 4, pp. 611-619, 2023. Abstract04-deferiprone_for_transfusional_iron_overload_in_sickle_cell_disease_and_other_anemias_open-label_study_of_up_to_3_year.pdf

Long-term safety and efficacy data on the iron chelator deferiprone in sickle cell disease (SCD) and other anemias are limited. FIRST-EXT was a 2-year extension study of FIRST (Ferriprox in Patients With Iron Overload in Sickle Cell Disease Trial), a 1-year, randomized noninferiority study of deferiprone vs deferoxamine in these populations. Patients who entered FIRST-EXT continued to receive, or were switched to, deferiprone. Altogether, 134 patients were enrolled in FIRST-EXT (mean age: 16.2 years), with mean (SD) exposure to deferiprone of 2.1 (0.8) years over the 2 studies. The primary end point was safety. Secondary end points were change in liver iron concentration (LIC), cardiac T2∗, serum ferritin (SF), and the proportion of responders (≥20% improvement in efficacy measure). The most common adverse events considered at least possibly related to deferiprone were neutropenia (9.0%) and abdominal pain (7.5%). LIC (mg/g dry weight) decreased over time, with mean (SD) changes from baseline at each time point (year 1, -2.64 [4.64]; year 2, -3.91 [6.38]; year 3, -6.64 [7.72], all P < .0001). Mean SF levels (μg/L) decreased significantly after year 2 (-771, P = .0008) and year 3 (-1016, P = .0420). Responder rates for LIC and SF increased each year (LIC: year 1, 46.5%; year 2, 57.1%; year 3, 66.1%; SF: year 1, 35.2%; year 2, 55.2%; year 3, 70.9%). Cardiac T2∗ remained normal in all patients. In conclusion, long-term therapy with deferiprone was not associated with new safety concerns and led to continued and progressive reduction in iron load in individuals with SCD or other anemias. The trial was registered at www.clinicaltrials.gov as #NCT02443545.

El‑Beshlawy, A., K. Abdel‑Azim, A. Abdel‑Salam, Y. M. M. Selim, F. Said, N. A. Gebril, E. Fateen, and P. Mistry, "Egyptian Gaucher disease type 3 patients: a large cohort study spanning two decades (journal article)", Journal of Rare Diseases, vol. 2, issue 7, pp. 1-6, 2023. s44162-023-00011-0-1.pdf