Abstract
Cancer dissemination and distant metastasis most frequently require the release of tumor cells into the blood circulation, both in solid tumors and most hematological malignancies, including plasma cell neoplasms. However, detection of blood circulating tumor cells in solid tumors and some hematological malignancies, such as the majority of mature/peripheral B-cell lymphomas and monoclonal gammopathies, has long been a challenge due to their very low frequency. In recent years, the availability of highly-sensitive and standardized methods for the detection of circulating tumor plasma cells (CTPC) in monoclonal gammopathies, e.g., next-generation flow cytometry (NGF), demonstrated the systematic presence of CTPC in blood in virtually every smoldering (SMM) and symptomatic multiple myeloma (MM) patient studied at diagnosis, and in the majority of patients with newly-diagnosed monoclonal gammopathies of undetermined significance (MGUS). These methods set the basis for further detailed characterization of CTPC vs. their bone marrow counterpart in monoclonal gammopathies, to investigate their role in the biology of the disease, and to confirm their strong impact on patient outcome when measured both at diagnosis and after initiating therapy. Here, we review the currently available techniques for the detection of CTPC, and determine their biological features, physiopathological role and clinical significance in patients diagnosed with distinct diagnostic categories of plasma cell neoplasms.
Highlights
Plasma cell neoplasms are an heterogenous group of end-stage antibody-producing B-cell disorders [1,2]
Even when highly-sensitive techniques are used, normal circulating plasma cells (PC) are undetectable at birth in cord blood
Flow cytometry has long been recognized as a well-suited methodology for the enumeration of circulating tumor plasma cells (CTPC) in blood of plasma cell neoplasms patients [20,22,122]
Summary
Plasma cell neoplasms are an heterogenous group of end-stage antibody-producing B-cell (i.e., plasma cell) disorders [1,2]. Circulating tumor plasma cells (CTPC) have long been detected in the blood of PCL patients [16,17,18], as well as in a significant fraction of MM [19,20,21,22], and to a lesser extent in MGUS cases [21,23]. We provide a detailed review of the currently available techniques for the detection of CTPC in patients with plasma cell neoplasms, their biological features, pathogenic role, and clinical relevance, with special focus on MGUS and MM patients. This is preceded by a brief overview of normal PC development. Relevant publications were reviewed and critically selected
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