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|C03= <div style="float: left; text-align: left; width: 25em; padding:1em;">'''Poor-Risk Cytogenetics|C04= <div style="float: left; text-align: left; width: 25em; padding:1em;">'''Salvage therapy''' </div>}} | |C03= <div style="float: left; text-align: left; width: 25em; padding:1em;">'''Poor-Risk Cytogenetics|C04= <div style="float: left; text-align: left; width: 25em; padding:1em;">'''Salvage therapy''' </div>}} | ||
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{{familytree | D01 | | | | | | D02 | | | | | | | | | D03 | | | | | | | | | | | | | | | | D04 | |D01= Select one of these therapies: <br> ❑ 1. Induction treatment: Cytarabine-based regimen + Daunorubicin. If a complete remission is achieved, postremission consolidation therapy as maintenance should be started: intermediate dose of Cytarabine) <br> ❑ 2.Investigational drugs(clinical trial): for cases aged younger than 60 years, a standard chemotherapy regimen including a backbone of Cytarabine + Anthracycline has been recommended. After complete remission, postremission therapy have to be | {{familytree | D01 | | | | | | D02 | | | | | | | | | D03 | | | | | | | | | | | | | | | | D04 | |D01= Select one of these therapies: <br> ❑ 1. Induction treatment: Cytarabine-based regimen + Daunorubicin. If a complete remission is achieved, postremission consolidation therapy as maintenance should be started: intermediate dose of Cytarabine) <br> ❑ 2.Investigational drugs(clinical trial): for cases aged younger than 60 years, a standard chemotherapy regimen including a backbone of Cytarabine + Anthracycline has been recommended. After complete remission, postremission therapy have to be regarded. | ||
|D02=Select one of these treatments: <br> | |D02=Select one of these treatments: <br> | ||
❑ 1. Investigational therapy: for patients older than 65 or have more comorbidities and high-risk illnesses or cases who cannot tolerate Cytarabine-based regimen + Daunorubicin, changing their regiments to an investigational therapy could be regarded. (administrate one chemotherapy drug or combine their treatment with non-intensive medications fitting with the patient such as decitabine, azacitidine) <br> ❑ 2. Induction treatment: Cytarabine-based regimen + Daunorubicin (could be suitable for young and elderly patients). If complete remission(CR) is achieved, postremission consolidation therapy as maintenance should be started to prevent relapse, including: <br> | ❑ 1. Investigational therapy: for patients older than 65 or have more comorbidities and high-risk illnesses or cases who cannot tolerate Cytarabine-based regimen + Daunorubicin, changing their regiments to an investigational therapy could be regarded. (administrate one chemotherapy drug or combine their treatment with non-intensive medications fitting with the patient such as decitabine, azacitidine). After complete remission, postremission therapy have to be regarded.<br> ❑ 2. Induction treatment: Cytarabine-based regimen + Daunorubicin (could be suitable for young and elderly patients). If complete remission(CR) is achieved, postremission consolidation therapy as maintenance should be started to prevent relapse, including: <br> | ||
:* Allogenic hematopoietic cell transplantation, which is the preferred treatment, or <br> | :* Allogenic hematopoietic cell transplantation, which is the preferred treatment, or <br> | ||
:* If the patient is younger than 60 years autologous hematopoietic cell transplantation is recommended, or <br> | :* If the patient is younger than 60 years autologous hematopoietic cell transplantation is recommended, or <br> | ||
Revision as of 04:41, 1 November 2020
| Acute leukemia Resident Survival Guide |
|---|
| Overview |
| Causes |
| FIRE |
| Diagnosis |
| Treatment |
| Do's |
| Don'ts |
Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1];
Synonyms and keywords: Acute lymphocytic leukemia, Acute myeloid leukemia, ALL, AML
Overview
Acute Leukemia is a malignancy of bone marrow myeloid and lymphoblastic precursor cells, in which these poorly differentiated hematopoietic cells proliferate rapidly. Hence, their accumulation would disrupt the performance of bone marrow to produce normal blood cells
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Causes
AML and ALL are life-threatening diseases, which would result in death if left untreated. In the majority of cases, etiology is not apparent.
Common Causes of AML
- Gene mutations:FLT3, IDHI, IDH2, KRAS, DNMT3A, NPM1
- Chromosomal translocations, deletions, and inversions
- Benzene or radiation exposure chronically[1]
Common Causes of ALL
- Radiation exposure:
- Genetic disorders; e.g., Down syndrome, ataxia-telangiectasia, Fanconi anemia
- Certain infections: e.g., HTLV-1
FIRE
A Focused Initial Rapid Evaluation (FIRE) should be performed to identify patients in need of immediate intervention.[5]
- Focused Initial Rapid Evaluation (FIRE) in AML:
Obtain patient's medical history and focus on these signs and symptoms: ❑ Fatigue ❑ Weight loss ❑ Anorexia ❑ Bone pain ❑ Bleeding ❑ Early satiety ❑ History of specific and chronic exposures such as alkylating agents, benzene, radiation, or previous chemotherapy ❑ Headache ❑ History of recurrent fever | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Examine the patient: ❑ Fever ❑ Ecchymosis ❑ Lymphadenopathy ❑ Splenomegaly ❑ Hepatomegaly ❑ Mediastinal mass ❑ Abnormalities in cranial nerve examination ❑ Skin Petechiae ❑ Testicular enlargement < | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Hematologic evaluation: ❑ CBD including platelets and WBCs) ❑ Uric acid, BUN, Cr, Liver function tests, bilirubin,Ca, P, Sodium, potassium, ❑ amylase, and lipase ❑ Lactate dehydrogenase ❑ PT, PTT ❑ D-dimer, fibrinogen ❑ Viral antibodies, (varicella-zoster, CMV), HSV-1 ❑ Peripheral blood smear | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Radiologic assessment: ❑ CXR (PA and lateral) ❑ PET or CT scan (if extramedullary disease is doubted based on symptoms and physical exam) ❑ CT, or MRI, and other imaging methods to diagnose ICH, brain or spinal cord tumors, and leptomeningeal disease (if patient presenting notable CNS signs and symptoms | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
❑ Bone marrow aspiration and biopsy | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
- Focused Initial Rapid Evaluation (FIRE) in ALL:
Take a precise medical history and focus on these signs and symptoms: ❑ Fatigue ❑ Anorexia ❑ Bone and joint pain ❑ Bleeding ❑ Weakness and lethargy ❑ History of prior exposures with alkylating agents, radiation, or previous chemotherapy (less prevalent than AML) ❑ Headache ❑ History of bleeding or unexplained bruising ❑ History of congenital syndroms ❑ Night sweats, weight loss and fever(B symptoms) ❑ Abdominal distention | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Examine the patient: ❑ Fever ❑ Tachycardia ❑ Mediastinal mass ❑ Lymphadenopathy ❑ Splenomegaly ❑ Hepatomegaly ❑ Abnormalities in cranial nerve examination ❑ Skin Petechiae ❑Testicular enlargement (rare) | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Hematologic evaluation: ❑ CBD including platelets and WBCs) ❑ Uric acid, BUN, Cr, Liver function tests, bilirubin ❑ Lactate dehydrogenase , potassium, phosphates, and calcium ❑ d-dimer, fibrinogen, PT, and PTT ❑ Peripheral blood smear | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Radiologic assessment: ❑ CXR (PA and lateral) to rule out mediastinal masses ❑ Brain CT scan and MRI with contrast if neurologic signs and symptoms have existed ❑ Scrotal ultrasound for assessing testicular involvement ❑ Echocardiogram or cardiac scan A whole body PET or CT scan when lymphoblastic lymphoma is doubted | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
❑ Bone marrow aspiration and biopsy | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Diagnosis
Diagnostic criteria of acute myeloid leukemia and acute lymphoblastic leukemia are similar to one another.
- According to the 2016 WHO criteria observing ≥20% blasts in the bone marrow biopsy or peripheral blood smear is diagnostic for AML. These genetic abnormalities in AML are diagnostic even with less than 20% marrow blasts: inv(16), t(16;16), t(8;21), and t(15;17).
- Presenting ≥20% of leukemic lymphoblasts in bone marrow aspirate and biopsy would prove ALL.
Treatment
Treatment of a patient with definitive AML | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Treating for the first time(new case) | Cases with relapsed/refractory AML | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Favorable-Risk Cytogenetics | Intermediate-Risk Cytogenetics | Poor-Risk Cytogenetics | Salvage therapy | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
| Select one of these therapies: ❑ 1. Induction treatment: Cytarabine-based regimen + Daunorubicin. If a complete remission is achieved, postremission consolidation therapy as maintenance should be started: intermediate dose of Cytarabine) ❑ 2.Investigational drugs(clinical trial): for cases aged younger than 60 years, a standard chemotherapy regimen including a backbone of Cytarabine + Anthracycline has been recommended. After complete remission, postremission therapy have to be regarded. | Select one of these treatments: ❑ 1. Investigational therapy: for patients older than 65 or have more comorbidities and high-risk illnesses or cases who cannot tolerate Cytarabine-based regimen + Daunorubicin, changing their regiments to an investigational therapy could be regarded. (administrate one chemotherapy drug or combine their treatment with non-intensive medications fitting with the patient such as decitabine, azacitidine). After complete remission, postremission therapy have to be regarded.
| D03 | D04 | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Do's
Don'ts
References
- ↑ Cancer Genome Atlas Research Network. Ley TJ, Miller C, Ding L, Raphael BJ, Mungall AJ; et al. (2013). "Genomic and epigenomic landscapes of adult de novo acute myeloid leukemia". N Engl J Med. 368 (22): 2059–74. doi:10.1056/NEJMoa1301689. PMC 3767041. PMID 23634996.