Your search keyword '"Hajjaj, Omar I."' showing total 9 results

1. Increasing rates of screening and treatment of iron deficiency in ambulatory patients with heart failure with reduced ejection fraction: a quality improvement cohort study

Author

Gewarges, Mena, primary, Mainland, Roslyn, additional, Wilkinson, Katherine, additional, Sklar, Jaime, additional, Gentilin, Andrew, additional, McLean, Bianca, additional, Hajjaj, Omar I, additional, Worme, Mali, additional, Lalonde, Spencer, additional, Patel, Raumil, additional, Lin, Yulia, additional, Callum, Jeannie, additional, and Poon, Stephanie, additional

Published

2024

2. Reducing blood product wastage through the inter‐hospital redistribution of near‐outdate inventory.

Author

Hajjaj, Omar I., Modi, Dimpy, Cameron, Tracy, Barty, Rebecca, Owens, Wendy, Heddle, Nancy, Zhang, Liying, Thompson, Troy, and Callum, Jeannie

Subjects

*BLOOD products, *BLOOD banks, *DO-not-resuscitate orders, *BLOOD proteins, *INVENTORIES

Abstract

Background: Hospital transfusion services order blood products to satisfy orders and maintain inventory levels during unexpected periods of increased blood demand. Surplus inventory may outdate before being allocated to a recipient. Blood product outdating is the largest contributor to blood wastage. Study Design: A province‐wide redistribution program was designed and implemented to redistribute near‐outdate plasma protein and related blood products from low‐usage to high‐usage hospitals. Program operations and details are described in this paper. Two transport container configurations were designed and validated for transport of all blood products. A cost‐analysis was performed to determine the effectiveness of this redistribution program. Results: A total of 130 hospital transfusion services contributed at least one near‐outdate blood product for redistribution between January 2012 and March 2020. These services redistributed 15,499 products through 3412 shipments, preventing the outdating of $17,570,700 CAD worth of product. Program costs were $14,900 for shipping and $30,000 for staffing. Failed time limits or non‐compliance with packing configurations resulted in $388,200 worth of blood products (97 shipments containing 816 products) being discarded. Courier transport delays was the most common reason (42/97; 43%) for transport failure. Conclusion: Redistributing near‐outdate blood products between hospitals is a feasible solution to minimize outdating. Despite heterogeneity of Canadian blood product inventory, all products (each with unique storage and transport requirements) were successfully redistributed in one of two validated and simple containers. Total operation costs of this program were small in comparison to the $17.6 million in savings associated with preventing the discard of outdated products. [ABSTRACT FROM AUTHOR]

Published

2024

3. Transfusion medicine curricular content for general pediatricians and pediatric subspecialists: A national multi‐specialty Delphi consensus study.

Author

Lieberman, Lani, Hajjaj, Omar I., Walsh, Catharine M., and Lin, Yulia

Subjects

*BLOOD transfusion, *DELPHI method, *PEDIATRICIANS, *BLOOD products, *STANDARDIZED tests

Abstract

Background: Although pediatric residents frequently order blood products, transfusion medicine (TM) education is both limited and unstandardized during postgraduate training. Using Delphi methodology, this study aimed to identify and prioritize which pediatric TM curricular topics are most important to inform postgraduate training in TM for general pediatricians and pediatric subspecialists. Methods: A national panel of experts iteratively rated potential curricular topics, on a 5‐point scale, to determine their priority for inclusion within a TM curriculum. After each round, responses were analyzed. Topics receiving a mean rating <3/5 were removed from subsequent rounds and remaining topics were resent to the panel for further ratings until consensus was achieved, defined as Cronbach α ≥ 0.95. At conclusion of the Delphi process, topics rated ≥4/5 were considered core curricular topics, while topics rated ≥3 to <4 were considered extended topics. Results: Forty‐five TM experts from 17 Canadian institutions and 12 subspecialties completed the first Delphi round and 31 completed the second. Fifty‐seven potential curricular topics were generated from a systematic literature review and Delphi panelists. Two survey rounds were completed before consensus was achieved. Seventy‐three topics in six domains reached consensus: 31 core curricular topics and 42 extended topics. There were no significant differences in ratings between TM and non‐TM specialists. Discussion: A multispecialty Delphi panel reached consensus in identification of curricular topics for pediatric resident physicians. These results set the stage to develop a pediatric TM curriculum that will be foundational for pediatric trainees to enhance learning and improve transfusion safety. [ABSTRACT FROM AUTHOR]

Published

2023

4. The burden of cyberattacks on blood management and conservation efforts

Author

Hajjaj, Omar I., primary, Modi, Dimpy, additional, Owens, Wendy, additional, Duybestyn, Andrew, additional, Thompson, Troy, additional, and Callum, Jeannie L., additional

Published

2022

5. Reconsidering sickle cell trait testing of red blood cell units allocated to children with sickle cell disease.

Author

Hajjaj, Omar I., Cserti‐Gazdewich, Christine, Dumevska, Letka, Hanna, Mirette, Lau, Wendy, and Lieberman, Lani

Subjects

*SICKLE cell trait, *SICKLE cell anemia, *ERYTHROCYTES, *BLOOD testing, *RED blood cell transfusion

Abstract

Background: Sickle cell trait (SCT) testing of red blood cell (RBC) units is sometimes performed to identify and divert units containing hemoglobin S (HbS). Recipients strategically guarded against this exposure include fetuses, neonates, and children with sickle cell disease (SCD). The clinical necessity of this practice is unclear. Study Design and Methods: A one‐year audit (2018) was performed at a pediatric tertiary care hospital that tests for SCT in RBC units prescribed to children with SCD and neonates. The impact of incorporating varying numbers of SCT RBC units in a single‐unit top‐up, partial‐manual red cell exchange, and automated erythrocytapheresis was modeled in four typical‐parameter age scenarios (2, 5, 10, and 18 years) sharing a high baseline HbS. Additionally, a survey assessing SCT testing practices was administered to Canadian pediatric hospital transfusion laboratories serving hemoglobinopathy programs. Results: Of 2268 donor RBC units tested, one was positive for SCT (0.04% [95% CI: 0.01%–0.24%]), at a cost of $19,384.56 CAD. The impact of SCT unit incorporation on lost HbS reduction was modest (Δ1%–3% [automated erythrocytapheresis] and Δ4%–15% [top‐up/partial manual exchange]). The survey (with all 13 sites responding) showed variable SCT testing practice; four (31%) do not test, four (31%) test for children with SCD, and six (46%) test for neonates. Conclusion: RBC SCT testing may be more costly than beneficial or necessary in children with SCD. As of 2019, our transfusion service has ceased SCT testing for this population. Further research in the fetal/neonatal populations is needed to overturn this entrenched practice. [ABSTRACT FROM AUTHOR]

Published

2023

6. Red blood cell changes due to cancer and cancer treatments: a narrative review

Author

Finnigan, Deirdre, Hajjaj, Omar I., and Othman, Maha

Published

2025

7. Immunohematology testing using umbilical cord blood: review of the literature, survey of practice and guidance development.

Author

Hajjaj, Omar I., Clarke, Gwen, and Lieberman, Lani

Abstract

Background: Following delivery, blood tests are performed on umbilical cord blood (CB) to avoid neonatal venipuncture. Despite widespread and longstanding CB testing, no guidelines exist to suggest which immunohematology tests should be performed on CB. Study design and methods: We performed a scoping review, surveyed national practice, and developed guidance statements concerning CB testing. Database searches identified relevant articles. A survey was sent to all Canadian hospitals and transfusion laboratories that perform perinatal testing. A national panel of experts was convened to develop guidance statements. Results: A total of 116 articles met the inclusion criteria and were summarized. Literature on CB testing is limited; few studies have investigated laboratory testing methodologies or validated CB test results with peripheral samples. The survey was completed by 580/597 institutions (97%); 85% were community hospitals and 16% had a neonatal intensive care unit. There is diversity in the types of CB tests performed and variability in practice. While most centers order appropriately, some laboratories routinely perform CB tests that are not clinically indicated (e.g., direct antiglobulin testing for all neonates) and other do not perform CB tests when results would be beneficial (e.g., phenotype on CB when mother has a clinically significant antibody). Fifteen guidance statements were developed. Discussion: This study highlights variability in CB testing, likely reflecting evidence gaps, methodology differences between studies, and lack of guidelines. CB tests should only be performed when indicated and validated on this sample type. The presented guidance statements aim to standardize practice and encourage judicious CB sampling. [ABSTRACT FROM AUTHOR]

Published

2022

8. Platelet and INR Thresholds and Bleeding Risk in Ultrasound Guided Percutaneous Liver Biopsy: A Before-After Implementation of the 2019 Society of Interventional Radiology Guidelines Observational Quality Improvement Study.

Author

DesRoche, Chloe, Callum, Jeannie, Scholey, Aiden, Hajjaj, Omar I., Flemming, Jennifer, Mussari, Ben, Tarulli, Emidio, Reza Nasirzadeh, Amir, and Menard, Alexandre

Subjects

*HEMORRHAGE prevention, *MEDICAL protocols, *HUMAN services programs, *RESEARCH funding, *BLOOD coagulation disorders, *DIGESTIVE system endoscopic surgery, *SCIENTIFIC observation, *RETROSPECTIVE studies, *BLOOD platelets, *NEEDLE biopsy, *INTERNATIONAL normalized ratio, *MEDICAL records, *ACQUISITION of data, *LIVER, *BLOOD transfusion, *QUALITY assurance, *PERIOPERATIVE care, PREVENTION of surgical complications

Abstract

Purpose: To evaluate if implementation of the 2019 Society of Interventional Radiology (SIR) guidelines for periprocedural management of bleeding risk in patients undergoing percutaneous ultrasound guided liver biopsy is associated with increased haemorrhagic adverse events, change in pre-procedural blood product utilization, and evaluation of guideline compliance rate at a single academic institution. Methods: Ultrasound guided percutaneous liver biopsies from (January 2019-January 2023) were retrospectively reviewed (n = 504), comparing biopsies performed using the 2012 SIR pre-procedural coagulation guidelines (n = 266) to those after implementation of the 2019 SIR pre-procedural guidelines (n = 238). Demographic, preprocedural transfusion, laboratory, and clinical data were reviewed. Chart review was conducted to evaluate the incidence of major bleeding adverse events defined as those resulting in transfusion, embolization, surgery, or death. Results: Implementation of the 2019 SIR periprocedural guidelines resulted in reduced guideline non-compliance related to the administration of blood products, from 5.3% to 1.7% (P =.01). The rate of pre-procedural transfusion remained the same pre and post guidelines at 0.8%. There was no statistically significant change in the incidence of bleeding adverse events, 0.8% pre guidelines versus 0.4% post (P = 1.0). Conclusion: Implementation of the 2019 SIR guidelines for periprocedural management of bleeding risk in patients undergoing percutaneous ultrasound guided liver biopsy did not result in an increase in bleeding adverse events or pre-procedural transfusion rates. The guidelines can be safely implemented in clinical practice with no increase in major adverse events. [ABSTRACT FROM AUTHOR]

Published

2024

9. Treatment differences and long-term outcomes in adults and children with Ewing sarcoma.

Author

Hajjaj OI, Corke L, Strahlendorf C, Hamilton SN, Feng X, and Simmons CE

Subjects

Humans, Male, Female, Retrospective Studies, Adult, Adolescent, Child, Young Adult, Middle Aged, British Columbia epidemiology, Child, Preschool, Bone Neoplasms mortality, Bone Neoplasms pathology, Bone Neoplasms drug therapy, Bone Neoplasms therapy, Survival Rate, Treatment Outcome, Aged, Sarcoma, Ewing mortality, Sarcoma, Ewing therapy, Sarcoma, Ewing pathology, Sarcoma, Ewing drug therapy

Abstract

Introduction: Ewing sarcoma is an aggressive malignancy primarily affecting children and adolescents. Limited research is available on treatment practices, clinical course, and survival in adults., Methods: A multi-institution retrospective cohort study of all adults (>18 years) and children (≤18 years) with Ewing sarcoma treated in British Columbia, Canada between January 01, 2000 and December 31, 2018., Results: One-hundred seven individuals (66 adults, 41 children) were included in the analysis. 5-year OS was 58 % in adults and 75 % in children. For individuals with local disease, 5-year OS was 74 % in adults and 84 % in children. Adult status was associated with impaired PFS (HR, 1.8; 95 % CI, 1.0 - 3.1, p=0.04) and OS (HR, 1.8; 95 % CI, 0.9 - 3.5; p=0.088). A Charlson Comorbidity Index (CCI) ≥3 was associated with impaired survival in adults and children (HR, 3.9, 95 % CI, 2.0 - 7.5; p=<0.001); baseline CCIs were not significantly different between groups. Most adults (61/66; 92 %) and all children (41/41; 100 %) received systemic treatment with no significant difference in mean lines of therapy, treatment modalities or agents. Most children received interval-compressed chemotherapy (35/41; 85 %) compared to adults (19/61; 29 %; p=<0.001). Interval-compression was not significantly associated with improved survival in adults with local disease (HR, 0.51; 95 % CI 0.1 - 2.3; p=0.373). Children more often initiated treatment within 28 days of diagnosis (31/33; 94 %) compared to adults (41/64; 64 %, p=0.001). Treatment within 28 days was associated with improved survival in the entire cohort (HR, 2.04 95 % CI, 1.1 - 3.9; p = 0.03). This association was preserved in subanalysis of individuals with local disease (HR, 5.4; 95 % CI, 1.9 - 15; p = 0.001) and only adults (HR, 5.3, 95 % CI, 1.7 - 17; p = 0.005)., Discussion: Survival for adults with Ewing sarcoma is inferior to children despite similarities in presentation, tumour characteristics and treatments. Further studies on the value of interval-compression in adults are required. Timely initation of treatment should be a priority for this disease., Competing Interests: Declaration of Competing Interest None of the study authors have a conflict of interest to declare., (Copyright © 2024. Published by Elsevier Ltd.)

Published

2024