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#1
Mon Apr 2, 2012, 07:48 PM
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The dysplasia part of myelodysplasia
What is meant by dysplasia in MDS? I know it means abnormal, but in what way? Are increased blast cell counts considered dysplasia? Genetic mutation such as deletion or trisomy? Or does it have to be how the blood cell is specifically formed and shaped?
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Caregiver to wife, 42 years old. Diagnosed MDS-RAEB II with auer rods and trisomy on chromosome 8. Currently under going induction chemo. 
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#2
Mon Apr 2, 2012, 08:34 PM
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Quote:
Myelo = bone marrow Dysplastic = abnormal cell growth or development Syndrome = group of symptoms, which together can define a disease Myelodysplastic Syndromes = a group of related diseases involving abnormal bone marrow cell growth or development An increased blast cell count is an important factor in classifying MDS too, but cell counts don't contribute to the name of the disease and not all MDS patients have increased blasts.
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#3
Mon Apr 2, 2012, 08:57 PM
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Thank you. This can be really confusing. As mentioned in another thread, on March 8, using a biopsy taken on Feb. 23, our doctor, a specialist at John Hopkins, diagnosised my wife with RAEB-II. She didn't say that any of the cells were dysplastic, just 8% or so blast cells. Also there was auer rods and trisomy 8. The doctor did not quite consider it leukemia because of the blast cell count, but was really on the fence about whether it really was MDS or AML. The doctor basically said whatever we call it, the treatment will be as if my wife does have AML.
Can you have MDS without the dysplasia, and can one have AML without the high blast count?
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Caregiver to wife, 42 years old. Diagnosed MDS-RAEB II with auer rods and trisomy on chromosome 8. Currently under going induction chemo.
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#4
Mon Apr 2, 2012, 10:51 PM
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My husband has been diagnosed with MDS without the dysplasia. We were told that sometimes it's diagnosed by exclusion.
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Catherine, wife of Bruce age 75; diagnosed 6/10/11 with macrocytic anemia, neutropenia and mild thrombocytopenia; BMB suggesting emerging MDS. Copper deficient. Currently receiving procrit and neuopogen injections weekly, B12 dermal cream and injections, Transfusions ~ 5 weeks.
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#5
Tue Apr 3, 2012, 12:35 PM
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One reason that it may be treated with induction chemotherapy like would be done with AML is the presence of auer rods. these are a little atypical in mds and is usually treated aggressively.
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MDS RCMD w/grade 2-3 fibrosis. Allo-MUD Feb 26, 2014. Relapsed August 2014. Free and clear of MDS since November 2014 after treatment with Vidaza and Rituxan. Experiencing autoimmune attack on CNS thought to be GVHD, some gut, skin and ocular cGVHD. Neuropathy over 80% of body.
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