Investigation and management of erythrocytosis

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madman

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Erythrocytosis refers to an erythrocyte count above the sex-specific normal range and can be subclassified into relative erythrocytosis, caused by a reduction in plasma volume (hemoconcentration), or absolute erythrocytosis, caused by increased erythrocyte mass. Primary erythrocytosis refers to the autonomous production of erythrocytes, typically from a myeloproliferative neoplasm (polycythemia vera [PV]). In contrast, secondary erythrocytosis is caused by a physiologically appropriate response to elevated serum erythropoietin levels. Up to 4% of ambulatory men and 0.4% of ambulatory women in Canada have erythrocytosis, based on hemoglobin levels greater than 165 g/L or 160 g/L, respectively.1 Differentiating PV from other causes of erythrocytosis is critical because early recognition and treatment of PV can prevent many of its vasomotor and thrombotic complications. Polycythemia vera is rare, with an incidence and prevalence of 0.84 and 22 per 100 000, respectively.2,3 Although the prevalence of secondary erythrocytosis is difficult to estimate, it is higher than that of PV. Secondary erythrocytosis affects 6%–8% of patients with chronic obstructive pulmonary disease4 and 2%–8% of patients with obstructive sleep apnea.5,6 In this review, we summarize a contemporary approach to differentiating PV from other causes of erythrocytosis and review the natural history, diagnosis, and management of PV (Box 1).




KEY POINTS

Primary erythrocytosis — or autonomous production of excess erythrocytes — most commonly occurs due to polycythemia vera (PV), a myeloproliferative neoplastic process that may be asymptomatic or may present with thrombosis, constitutional or vasomotor symptoms, or splenomegaly.

Secondary erythrocytosis, which is more common than PV, has a broad differential diagnosis that includes hypoxic lung disease, cyanotic congenital heart disease, medications (e.g., testosterone) and erythropoietin-producing malignant disorders.

Differentiating between PV and secondary erythrocytosis requires clinical evaluation and specialized investigations including measurement of the serum erythropoietin level and Janus kinase 2 mutation testing.

To reduce the risk of thrombosis, most patients with PV are treated with low-dose acetylsalicylic acid and phlebotomy to achieve a target hematocrit value of less than 0.45, whereas patients at high risk for thrombosis may receive cytoreductive therapy.

Treatment of secondary erythrocytosis should be directed at the underlying cause, and phlebotomy is not routinely recommended




Box 2: Causes of secondary erythrocytosis14

Hypoxia-driven

Generalized tissue hypoxia

• Smoking
• Carbon monoxide poisoning
• Hypoxic lung disease
• Obstructive sleep apnea
• Right to left cardiopulmonary shunt (e.g., cyanotic congenital heart disease)
• High altitude Local renal hypoxia
• Renal artery stenosis
• Hydronephrosis
• Renal cysts (polycystic kidney disease) Drug-associated
• Testosterone
• Erythropoietin Pathologic erythropoietin production
• Renal cell carcinoma
• Hepatocellular carcinoma
• Cerebellar hemangioblastoma
• Uterine leiomyomata
• Parathyroid carcinoma
• Meningioma Miscellaneous
• Erythrocytosis after renal transplantation
Idiopathic erythrocytosis*


*Diagnosis of exclusion





Box 3: World Health Organization 2016 polycythemia vera diagnostic criteria16

Diagnosis of polycythemia vera requires all 3 major criteria OR the first 2 major criteria and the minor criterion

Major criteria

• Hemoglobin level > 165 g/L in men, > 160 g/L in women OR hematocrit > 0.49 in men, > 0.48 in women OR increased erythrocyte mass

• Bone marrow biopsy showing hypercellularity for age with trilineage growth (panmyelosis) including prominent erythroid, granulocytic and megakaryocytic proliferation with pleomorphic, mature megakaryocytes*

• Presence of JAK2 V617F or JAK2 exon 12 mutation Minor criterion

• Subnormal serum erythropoietin level


*Bone marrow biopsy is not required for patients with sustained absolute erythrocytosis, defined as a hemoglobin level greater than 185 g/L in men (hematocrit 0.55) or greater than 165 g/L in women (hematocrit 0.50) if the third major criterion and the minor criterion are met







Conclusion

Secondary erythrocytosis can be distinguished from PV in most patients with a focused clinical evaluation and, where available, determination of the erythropoietin level and JAK2 V617F mutation testing. The goals of treatment in PV are to alleviate symptoms reduce the risk of thromboembolism and monitor patients for transformation to myelofibrosis or acute leukemia. The majority of patients with PV should be treated with low-dose ASA and phlebotomy to achieve a target hematocrit value of less than 0.45. Cytoreduction, most commonly with hydroxyurea, should be considered in patients at high risk for thrombosis. Treatment of secondary erythrocytosis should be directed at the underlying cause.
 

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madman

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Screenshot (1757).png

Figure 1: Practical diagnostic approach to erythrocytosis. *Some clinicians order determination of the erythropoietin level and JAK2 V617F mutation testing concurrently in settings when there is a high probability of diagnosing polycythemia vera. †Bone marrow biopsy is required to meet the World Health Organization 2016 diagnostic criteria16 if the hemoglobin level is less than 185 g/L (hematocrit 0.55) in men or less than 165 g/L (hematocrit 0.50) in women.
 

madman

Super Moderator
Screenshot (1758).png

Screenshot (1759).png

Figure 2: Bone marrow biopsy specimen of a patient with polycythemia vera. (A) Hypercellularity for age and panmyelosis (expansion of all myeloid elements of the bone marrow) (hematoxylin-eosin, ×40 magnification). (B) Panmyelosis and pleomorphic megakaryocytes (hematoxylin-eosin, ×200 magnification). Images courtesy of Dr. Catherine Ross, Pathology and Molecular Medicine, Juravinski Hospital, Hamilton, Ontario.
 
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