Myelodysplastic syndrome

Myelodysplastic syndrome (MDS) is a hematopoetic disease caused by a hematopoetic stem cell mutation that results in the formation of a pathological clone of cells of one or more blood lines. We can find pancytopenia in the peripheral blood, on the contrary, the bone marrow is normo- or hypercellular with signs of dysplasia. In about 10 % of cases, the bone marrow can also be hypocellular and difficult to distinguish from aplastic anemia. In the late stage, MDS can progress to acute myeloid leukemia. The incidence is 4.5 patients per 100,000 inhabitants. The incidence of patients with MDS increases in people over 60 years of age.

Etiology[edit | edit source]

Based on the action of pathological insults (virus, toxin, radiation, exposure to mutagen), a mutation of the hematopoetic stem cell occurs, as well as a pathological immune response, which leads to the apoptosis of more mature cells from the hematopoetic line.

Clinical picture[edit | edit source]

anemia: anemic syndrome (fatigue, paleness, shortness of breath);
leukocytopenia: infection;
thrombocytopenia : bleeding manifestations.

Laboratory finding[edit | edit source]

In the peripheral blood, cytopenia (of one or more blood lines) is expressed differently, in the later stages, blastic variants of cells are washed out into the peripheral blood. In the bone marrow, the cells are morphologically and dysplastically changed, there are signs of cellular maturation (blasts) and sideroblasts.

WHO classification[edit | edit source]

Refractory cytopenia with dysplasia of one line RCUD

refractory anemia – RA
refractory neutropenia – RN
refractory thrombocytopenia – RT

Refractory anemia with annular sideroblasts - RARS
Refractory cytopenia with multilineage dysplasia – RCMD
Refractory anemia with excess blasts 1 - RAEB-1
Refractory anemia with excess blasts 2 - RAEB-2
MDS unclassified – MDS-U
MDS with isolated 5q deletion

Treatment[edit | edit source]

supportive treatment: transfusion of erythrocytes, platelets, administration of vitamin B, chelating agents;
substances inhibiting apoptosis: growth factors (erythropoietin, G-SCF);
immunosuppressive and immunomodulating substances: corticosteroids + cyclosporine A , lenalidomide;
hypomethylating agents – 5-azacytidine, decitabine;
chemotherapy:
- monoterapie – hydroxyurea, etoposid;
- combined – anthracyclines + cytosine;
allogeneic hematopoietic cell transplantation.

Prognosis[edit | edit source]

The prognosis for patients with MDS is variable. Negative prognostic factors are a high number of circulating blasts (patients with more than 20 % blasts are classified as AML), dysplasia of all three lines, complex karyotype changes and abnormalities of the 7th chromosome. The most common causes of morbidity and mortality in patients with MDS are: progression to AML, severe neutropenia or thrombocytopenia, iron overload, and cardiac disease. Average time of survival is 2 years.

Summary video[edit | edit source]

<mediaplayer width="500" height="300">https://www.youtube.com/watch?v=fT_NTuZSbkQ</mediaplayer>

Sources[edit | edit source]

External links[edit | edit source]

Literature[edit | edit source]

ČEŠKA, Richard – TESAŘ, Vladimír. Interna. 132. edition. Triton, 2012. ISBN 978-80-7387-629-6.

NEČAS, Emanuel – ŠULC, Karel – VOKURKA, Martin. Patologická fyziologie orgánových systémů. Část I. 1. edition. Karolinum, 2006. 0 pp. ISBN 978-80-246-0615-6.