Prof Bowen delivering a talk for Prof Platzbecker on novel approaches to cytopenias in MDS #BSH2019
Around 30% of patients will respond to Eprex and license for MDS came last year medicines.org.uk/emc/product/11…
Darbepoietin didn't meet its primary endpoint and so not licensed but real world experience is that both are in use for anaemia in MDS #BSH2019
Median duration of response is 17 months. Sideroblastic patients respond less well. If EPO raised and transfusion dependent, only 10% will respond. All others should have a therapeutic trial. Even those with RAEB-1 may continue to respond for a good time #BSH2019
Luspatercept is a GDF11 inhibitor which removes suppression of erythropoiesis without having an effect on bone metabolism #BSH2019
Luspatercept reduces red cell and ESA requirements. SF3B1 mutated patients and those with sideroblastic patients respond better #BSH2019
Phase 3 trial MEDALIST of luspatercept every 21d vs placebo in transfusion dep pts. Del 5q and >5% blasts excluded. 226 patients randomised #BSH2019
Primary endpoint of transfusion independence met in 37.9% patients vs 13.2% in the placebo arm, p<0.0001. Improvement continues even beyond 8 weeks. Results presented at ASH and full paper awaited #BSH2019 ascopost.com/News/59528
Other novel treatments in development for anaemia in MDS include imetelstat - telomerase inhibitor. Response rates approx 35% response, independent of EPO baseline #BSH2019
Spliceosome inhibitors: mutations such as SF3B1 are common in MDS and subtypes. H3B-8800 appears effective but carries potentially for retinal and liver toxicity #BSH2019
Eltrombopag increases platelet count in low risk MDS thelancet.com/journals/lanha…
Romiplostim trial did not show increased survival but did demonstrate fewer bleeding events
Neither licensed in MDS currently #BSH2019
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I had a personal request to do a tweetorial for the #haemSpRs on haemovigilance. Here goes. A #blooducation 🧵
Haemovigilance is a systematic surveillance of adverse reactions and adverse events related to transfusion’ with the aim of improving transfusion safety. transfusionguidelines.org/transfusion-ha…
We are very lucky in the UK to have @SHOTHV1, one of the first in the world to collate adverse events relating to transfusion - since the 1990s.
This morning I met with the chair and vice chair of the Midlands Regional Transfusion Committee, the Midlands Patient Blood Management Practitioner and the Customer Services Manager. What are their roles and what does the RTC do?
A #blooducation 🧵
RTCs serve to bring together Hospital Transfusion Committees to discuss best practice, implement new guidance and provide educational resources and events. They are run by clinicians and scientists working in hospitals, supported by @NHSBT.
Teaching our incoming haematology doctors today about transfusion in haematology patients. So who needs irradiated blood and why? A #blooducation🧵
All blood in the UK is leucocyte reduced (except granulocytes, but that’s another story). Despite this, a unit of red cells or platelets can have around a million residual white cells, mostly lymphocytes.
Every doctor starting in a new trust does transfusion training as part of their mandatory training. But why?
50ml ABO incompatible blood can kill a patient. ABO antibodies are naturally occurring (“everyone” has them) and they are IgM; they can activate complement and cause *immediate* intravascular haemolysis, causing release of free haem, endothelial activation, renal failure and DIC.
In most hospitals, blood banks require 2 samples (one may be historic) before releasing group specific (non-O) blood for a patient. This is to increase the chances of identifying a *wrong blood in tube* (pt whose blood's in the tube is not the pt whose details are on the outside)
It can be difficult to know where to start with transfusion – you can’t go on a ward round to find patients. BUT you do start with lab induction and your helpful #BMSes will show you around.
Excellent session on emergency paediatric transfusion #AABB20. Cyril Jacquot talking on pre hospital transfusion and summarising the literature.
28 day mortality following haemorrhage is higher in children than adults (unpublished data and substudies from PROPPR and PROMMTT)
Observational studies of large numbers of patients but with only very small numbers of paediatric patients suggest that pre hospital blood is not associated with an excess of transfusion reactions and in some studies is thought to have improved survival.
Whole blood, group O, high titre neg, used in paediatrics in Pittsburgh appears to be safe with no haemolysin-mediated haemoylsis in non group O patients (Leeper et al JAMA Pediatrics 2018) ncbi.nlm.nih.gov/pmc/articles/P…