Acute Leukemia Presentation with DIC




© Springer International Publishing Switzerland 2017
Robert C. Hyzy (ed.)Evidence-Based Critical Care10.1007/978-3-319-43341-7_71


71. Acute Leukemia Presentation with DIC



Laurie A. Manka  and Kenneth Lyn-Kew 


(1)
Division of Pulmonary, Critical Care and Sleep Medicine, Department of Medicine, National Jewish Health, Denver, CO, USA

 



 

Laurie A. Manka (Corresponding author)



 

Kenneth Lyn-Kew



Keywords
AMLAPMLDICThrombocytopeniaT(15;17)ATRA



Case Presentation


A 36 year old female presented to the hospital with tongue swelling and bleeding after she bit her tongue. Due to worsening swelling of her tongue, she was emergently intubated in the emergency department and transferred to the ICU for further management of her airway. Her recent history was significant for fatigue, menorrhagia, multiple “colds” and sore throats, and recurrent infections of her umbilical piercing. On exam she was noted to have shotty cervical lymphadenopathy and a swollen tongue without evidence of lip swelling. There was evidence of cellulitis around her umbilical piercing, which was subsequently removed. CT neck demonstrated no abscess of the posterior oropharynx but was limited in ability to evaluate the tongue due to the presence of the endotracheal tube. Initial laboratory work showed a pancytopenia with a white blood cell count of 4.0 × 103/μL, hemoglobin 7.5 g/dl, and platelets 116 × 103/μL. Her peripheral smear showed evidence of “rare” blasts. Her coagulation derangements consisted of a prolonged prothrombin time (PT) of 16.1 s, INR of 1.32, partial thromboplastin time (PTT) of 36.5 s. Her D-dimer was greater than the upper level of detection at 500 μg/dL. Fibrin split products were >20 μg/dL, and her Fibrinogen was 344 mg/dL. Because of the patient’s pancytopenia, a bone marrow biopsy was obtained and showed a hypercellular marrow with markedly increased blasts, accounting for 95 % of the total cells. Chromosomal analysis demonstrated t(15;17) rearrangement.


Question

What is the diagnosis?


Answer

DIC in the setting of Acute Promyelocytic Leukemia (APML or AML M3)

Acute Promyelocytic leukemia (APML) is a form of acute myelocytic leukemia (AML), comprising approximately 10 % of AMLs diagnosed. APML is specifically characterized by a reciprocal translocation between the retinoic acid receptor-alpha (RAR-α) gene on chromosome 17 and the PML gene on chromosome 15. This rearrangement is known as t(15;17). APML often acutely presents clinically with extensive bleeding diathesis requiring ICU admission at the time of diagnosis [1]. Up to 15 % of APMLs will present with DIC. This can be due to the disease itself or the effect of undergoing induction chemotherapy [2, 3].

In the setting of acute APML, the extensive bleeding characteristics are due to hyper fibrinolysis driven primarily by fibrinolytics such as u-PA, t-PA, as well as protease elastase and chemotrypsin [4, 5] which are found in high levels in leukemic blast cells [4, 5]. The over production of these fibrinolytics in the setting of profound thrombocytopenia due to bone marrow dysfunction yield the profound bleeding disorder [1].

DIC is also closely associated with the induction therapy in APML. Treatment of APML consists primarily of use of All-trans-retinoic acid (ATRA). ATRA promotes differentiation of leukemic blasts. This process can transiently worsen DIC by consumption of pro-coagulation factors, namely Tissue Factor (TF) and Cancer Procoagulant (CP) [6, 7]. However, within approximately 48 h, as the leukemic blast burden improves so do the markers of DIC.


Principles of Management



Confirm the Diagnosis of AML


AML is a group of hematopoietic neoplasms arising from the precursors of the myeloid cell lines. AML is the most common cause of acute leukemia in adults, with approximately 20,000 cases annually and 10,000 deaths [8]. AML is classified based on specific genetic abnormalities (as in this case), or if it does not fit a specific genetic abnormality, by cell morphology.

Clinical features of AML are primary related to pancytopenia and high cellular turnover in proliferating leukemia cells. These include fatigue, weakness and pallor due to anemia, fever due to immune dysregulation and subsequent infection, infiltrative skin lesions (leukemia cutis), acute neutrophilic dematosis (Sweet syndrome) and petechiae and fundal hemorrhages due to thrombocytopenia or, as in the above case, DIC. Additionally patients may present with tumor lysis syndrome, characterized by hypocalcemia, hyperuricemia, hypokalemia and/or hyperphosphatemia. Circulating leukemic blast cells are frequently found on peripheral smear.

Confirmation of the diagnosis of AML is made by bone marrow aspiration or bone marrow biopsy, particularly when aspiration fails to yield the diagnosis. The diagnosis requires documentation of bone marrow infiltration and the myeloid origin of the cells, with the exception of genetic abnormalities specific to AML such as the t(15;17) in this case.


Make the Correct Diagnosis of DIC



Differential Diagnosis of DIC


The first step to treatment of DIC in the ICU is correct diagnosis. The differential diagnosis of DIC often revolves around discovery of new thrombocytopenia. The differential diagnosis of acute thrombocytopenia in the ICU is extensive and includes a multitude of commonly seen disorders in the ICU.

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Jul 20, 2017 | Posted by in Uncategorized | Comments Off on Acute Leukemia Presentation with DIC

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