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Author(s):  
Marouane El Midaoui ◽  
Mohammed Qbadou ◽  
Khalifa Mansouri

Multiple diseases require a blood transfusion on daily basis. The process of a blood transfusion is successful when the type and amount of blood is available and when the blood is transported at the right time from the blood bank to the operating room. Blood distribution has a large portion of the cost in hospital logistics. The blood bank can serve various hospitals; however, amount of blood is limited due to donor shortage. The transportation must handle several requirements such as timely delivery, vibration avoidance, temperature maintenance, to keep the blood usable. In this paper, we discuss in first section the issues with blood delivery and constraint. The second section present routing and scheduling system based on artificial intelligence to deliver blood from the blood-banks to hospitals based on single blood bank and multiple blood banks with respect of the vehicle capacity used to deliver the blood and creating the shortest path. The third section consist on solution for predicting the blood needs for each hospital based on transfusion history using machine learning and fuzzy logic. The last section we compare the results of well-known solution with our solution in several cases such as shortage and sudden changes.


2021 ◽  
Vol 73 ◽  
pp. 352-354
Author(s):  
Jatin Agrawal ◽  
Ashish Kumar ◽  
Anil Arora

Congenital venous malformations (VMs) are rare cause of gastrointestinal (GI) bleed in children. Blue rubber bleb nevus syndrome characterized by VMs in GI tract and skin affect at early age in life. Diagnosis is based on typical skin lesion and history of recurrent GI bleed. In this article, we presented a similar case of young girl with typical skin lesion and recurrent GI bleed requiring multiple blood transfusions presenting our department. She was subjected to surgical treatment and endoscopy therapy due to failure of conservative therapy. This case report depicts importance of typical clinical features of rare diseases.


2021 ◽  
Vol 23 (Supplement_6) ◽  
pp. vi20-vi21
Author(s):  
Pamela Jackson ◽  
Minjee Kim ◽  
Andrea Hawkins-Daarud ◽  
Kyle Singleton ◽  
Afroz Mohammad ◽  
...  

Abstract Choosing effective chemotherapies for intravenous delivery to brain tumors is challenging, especially given the protective nature of the blood brain barrier (BBB). Connecting drug distribution to non-invasive, pre-surgical magnetic resonance imaging (MRI) could allow for predictive insight into drug distribution. In a previous study, we found that T2Gd images were predictive of a low BBB penetrant drug (Cefazolin), and FLAIR images were predictive of a high BBB penetrant drug (Levetiracetam). While these results are promising, we further seek to explore how advanced MRI sequences might inform image-based models of drug distribution. Prior to surgery, we acquired advanced dynamic contrast enhanced (DCE) and diffusion weighted imaging (DWI) MRI sequences for eight brain tumor patients (7 gliomas and 1 metastatic adenocarcinoma) in addition to the anatomic MRIs. All resulting quantitative maps and acquired images were co-registered. Prior to incision, patients received injections of cefazolin and levetiracetam. Next, multiple blood samples and biopsies were collected during surgery. Biopsies and plasma samples were analyzed for drug concentration using liquid chromatography mass spectrometry (LCMS), and biopsy drug levels were reported as Brain-Plasma Ratio (BPR). Mean image intensity was extracted from a 15x15 voxel window surrounding the biopsy location. We performed linear regression analyses to determine which combination of images were predictive of BPR. We found that considering quantitative imaging improved our initial ability to predict BPR for both drugs. For cefazolin, the third diffusion tensor eigenvalue (L3) map was significantly correlated with BPR (p< 0.001, R2= 0.36). For levetiracetam, the best model consisted of a combination of images and maps with the L3 map and the isotropic diffusion map (P) being the most influential (p= 0.001, R2= 0.63). Advanced MRI-based modeling is a promising tool for forecasting drug distribution in brain tumors and could be of great importance for understanding efficacy and selecting therapeutic strategies.


2021 ◽  
Vol 8 (Supplement_1) ◽  
pp. S805-S806
Author(s):  
Lauren E Gentles ◽  
Leanne P Kehoe ◽  
Katharine D Crawford ◽  
Kirsten Lacombe ◽  
Jane Dickerson ◽  
...  

Abstract Background Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection elicits antibodies (Abs) that bind several viral proteins such as the spike entry protein and the abundant nucleocapsid (N) protein. We examined convalescent sera collected through 6 months (~24wks) post-SARS-CoV-2 infection in children to evaluate changes in neutralization potency and N-binding. Methods Outpatient, hospitalized, and community recruited volunteers < 18 years with COVID-19 were enrolled in a longitudinal study at Seattle Children’s Hospital. Analysis includes symptomatic and asymptomatic children with laboratory-confirmed SARS-CoV-2 infection who provided blood samples at approximately 4wks (range: 2-18wks, IQR:4-8wks) and 24 wks (range: 23-35wks, IQR:25-27wks) after diagnosis. We measured neutralizing Ab using an in-house pseudoneutralization assay and anti-N binding Ab using the Abbott Architect assay. Results Of 32 children enrolled between April 2020 and January 2021, 27 had no underlying immunocompromised state and 25 of these 27 children had symptomatic disease. Ten of 27 had a > 2-fold decrease neutralization titers between 4 and 24wks (most were < 10-fold); 12 had < 2-fold change; and 5 had neutralization titers that increased > 2-fold over time (Fig. 1A). All but one of these 27 children had detectable neutralizing activity at 24wks. Anti-N Abs were assessed for 25 children at 4wks and 17 children at 24wks (data pending for 14 samples); all children with paired samples had a > 1.75-fold Abbott index reduction at 24wks, and 5 children had no detectable anti-N Abs by 24wks (Fig. 2A). An additional 5 children with symptomatic disease had complicating immunosuppression or multiple blood transfusions; 2 had decreasing neutralizing titers, 2 increased, and 1 had no change (Fig. 1B). Anti-N Abs were undetectable for one child by 24wks (data pending for 4 samples) (Fig. 2B). No participants received COVID-19 vaccine. Figure 1. Pseusoneutralization titers in children over time. Figure 2. Nucleocapsid-binding antibody titers in children over time. Conclusion We show neutralizing Abs wane to a small degree over 24wks post-SARS-CoV-2 infection and remain detectable in most children. In contrast, anti-N Abs decreased, becoming undetectable in some children by 24wks. These findings add to understanding of the natural history of SARS-CoV-2 immunity in children. * This study was supported by CDC BAA75D301-20-R-67897 Disclosures Jesse Bloom, PhD, Flagship Labs 77 (Consultant)Moderna (Consultant) Janet A. Englund, MD, AstraZeneca (Consultant, Grant/Research Support)GlaxoSmithKline (Research Grant or Support)Meissa Vaccines (Consultant)Pfizer (Research Grant or Support)Sanofi Pasteur (Consultant)Teva Pharmaceuticals (Consultant)


2021 ◽  
Vol 15 (10) ◽  
pp. 3384-3386
Author(s):  
Tasneem Kousar ◽  
Rizwana Qureshi ◽  
Bhag Chand Lohano ◽  
Chetan Das ◽  
Sonika Hotwani

Objective: To evaluate the frequency of hepatitis C virus and hepatitis B virus among children underwent multiple blood transfusions at tertiary care Hospital. Methodology: This cross-sectional retrospective study was conducted at paediatrics department of Liaquat University of Medical and Health Sciences. All the children below the age of 12 years, both gender and presented with history of multiple blood transfusions due different hematological disorders at paediatrics department were included. After taking complete medical history, all the children underwent screening for hepatitis B virus and hepatitis C virus. After taking verbal informed consent a 3 ml or 5ml blood sample was taken from each case and sent to the Hospital diagnostic Laboratory for the HCV and HVB screening. All the data was collected by the self-made study proforma. Data analysis was done using SPSS version 20. Results: A total of 102 children were studied. The mean age of the children was 8.57+2.97 years and average hemoglobin level was 9.26+2.91. Males were in the majority 74(72.5%). Most of the children 42(41.2%) had thalassemia. The frequency of HBV was 5.9% and HCV was 33.3% among children of multiple blood transfusions. The frequency of HCV and HBV were insignificant according to gender (p->0.05) and statistically significant according to numbers of blood transfusion (p-<0.05). Conclusion: It was concluded that the frequency of HCV infection was high among children of multiple blood transfusions. Key words: TTI, HCV, HBV, seropositivity


Author(s):  
John B. Keven ◽  
Michelle Katusele ◽  
Rebecca Vinit ◽  
Daniela Rodríguez-Rodríguez ◽  
Manuel W. Hetzel ◽  
...  

Nonrandom selection and multiple blood feeding of human hosts by Anopheles mosquitoes may exacerbate malaria transmission. Both patterns of blood feeding and their relationship to malaria epidemiology were investigated in Anopheles vectors in Papua New Guinea (PNG). Blood samples from humans and mosquito blood meals were collected in villages and human genetic profiles (“fingerprints”) were analyzed by genotyping 23 microsatellites and a sex-specific marker. Frequency of blood meals acquired from different humans, identified by unique genetic profiles, was fitted to Poisson and negative binomial distributions to test for nonrandom patterns of host selection. Blood meals with more than one genetic profiles were classified as mosquitoes that fed on multiple humans. The age of a person bitten by a mosquito was determined by matching the blood-meal genetic profile to the villagers’ genetic profiles. Malaria infection in humans was determined by PCR test of blood samples. The results show nonrandom distribution of blood feeding among humans, with biased selection toward males and individuals aged 15–30 years. Prevalence of Plasmodium falciparum infection was higher in this age group, suggesting males in this age range could be super-spreaders of malaria parasites. The proportion of mosquitoes that fed on multiple humans ranged from 6% to 13% among villages. The patterns of host utilization observed here can amplify transmission and contribute to the persistence of malaria in PNG despite efforts to suppress it with insecticidal bed nets. Excessive feeding on males aged 15–30 years underscores the importance of targeted interventions focusing on this demographic group.


2021 ◽  
Vol 22 (18) ◽  
pp. 9677
Author(s):  
Anna Gluba-Brzózka ◽  
Beata Franczyk ◽  
Magdalena Rysz-Górzyńska ◽  
Robert Rokicki ◽  
Małgorzata Koziarska-Rościszewska ◽  
...  

Thalassemia, a chronic disease with chronic anemia, is caused by mutations in the β-globin gene, leading to reduced levels or complete deficiency of β-globin chain synthesis. Patients with β-thalassemia display variable clinical severity which ranges from asymptomatic features to severe transfusion-dependent anemia and complications in multiple organs. They not only are at increased risk of blood-borne infections resulting from multiple transfusions, but they also show enhanced susceptibility to infections as a consequence of coexistent immune deficiency. Enhanced susceptibility to infections in β-thalassemia patients is associated with the interplay of several complex biological processes. β-thalassemia-related abnormalities of the innate immune system include decreased levels of complement, properdin, and lysozyme, reduced absorption and phagocytic ability of polymorphonuclear neutrophils, disturbed chemotaxis, and altered intracellular metabolism processes. According to available literature data, immunological abnormalities observed in patients with thalassemia can be caused by both the disease itself as well as therapies. The most important factors promoting such alterations involve iron overload, phenotypical and functional abnormalities of immune system cells resulting from chronic inflammation oxidative stress, multiple blood transfusion, iron chelation therapy, and splenectomy. Unravelling the mechanisms underlying immune deficiency in β-thalassemia patients may enable the designing of appropriate therapies for this group of patients.


2021 ◽  
Vol 2 (2) ◽  
pp. 283-289
Author(s):  
P. N. Shrestha

Over90% of recipients of HIV infected blood will seroconvert. In the Region 368 cases were due to transmission through blood or blood products. With establishment of HIV screening facilities, the proportion of AIDS cases due to blood transmission has decreased. AIDS due to blood transmission will continue to occur due to the time lag between the occurrence of HIV infection and appearance of AIDS. HIV seroprevalence among recipients of multiple blood transfusions decreased from 270 per 10 000 in 1987-89 to 7 per 10 000 in 1995. Effective methods are available for prevention of HIV transmission through blood, but antigen and PCR tests are expensive and not recommended for screening of blood donations in developing countries


2021 ◽  
Vol 14 (8) ◽  
pp. e243421
Author(s):  
Rahul Nema ◽  
Abhinav Sengupta ◽  
Arvind Kumar ◽  
Naveet Wig

A 40-year-old woman presented to our emergency department in an altered state following a generalised tonic-clonic seizure. On regaining consciousness, she gave a history of bleeding tendencies and menorrhagia, fatigue, nausea, vomiting and appetite loss for a long time. She had received multiple blood transfusions in the last 10 years. Investigations revealed severe hyponatraemia, transaminitis and pancytopenia, which showed cyclical fluctuations in the hospital. Hyponatraemia was attributed to a central cause owing to secondary hypothyroidism and hypocortisolism on evaluation. A diagnosis of cyclical thrombocytopenia was made by logging the trends of blood cell lines and applying the Lomb-Scargle test. Liver biopsy showed features of transfusion hemosiderosis explaining transaminitis. All of the haematological abnormalities and clinical symptoms resolved on thyroxine and corticosteroid replacement, suggesting causal association hypopituitarism with cyclical thrombocytopenia


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