# Cryoglobulinemia, monoclonal and mixed cryoglobulinemia syndromes, cryoglobulinemic vasculitis: a proposal for comprehensive nomenclature and definition

**Authors:** Clodoveo Ferri, Laura Gragnani, Anna Linda Zignego, Dilia Giuggioli

PMC · DOI: 10.3389/fimmu.2026.1754012 · 2026-02-20

## TL;DR

The paper proposes a unified naming system for cryoglobulinemia to clarify its different forms and improve diagnosis and treatment.

## Contribution

The paper introduces a comprehensive nomenclature and definition system for cryoglobulinemia and its related syndromes.

## Key findings

- Monoclonal and mixed cryoglobulinemia are distinct clinical entities with different associations and manifestations.
- Standardized definitions are needed to improve diagnostic accuracy and enable better clinical studies.
- New antiviral treatments have reduced virus-related mixed cryoglobulinemia in developed countries.

## Abstract

Cryoglobulinemia indicates the reversible, cold-dependent precipitation of immunoglobulins (Ig), which may be monoclonal (MoC) or mixed IgG–IgM (MC). Although this in vitro phenomenon is relatively frequent, only a minority of cases develop clinically relevant manifestations, often falling within lymphoproliferative, autoimmune, or infectious disease domains. This complexity highlights the need for clearer nomenclature and definition systems.

The term “cryoglobulinemia” is often used interchangeably to describe either simple laboratory finding, asymptomatic cryo-Ig precipitation (MoC or MC) or corresponding clinical syndromes (MoCs or MCs). This overlap creates ambiguity, hinders expert communication, and complicates the comparison of clinical studies. A standardized nomenclature is therefore essential to define disease subsets, establish boundaries with related conditions, and enable reliable data collection and multicenter analyses.

When cryoglobulins are detected, the cryoprecipitate must be isolated and defined as MoC or MC, followed by a systematic clinical and laboratory assessment to identify potential underlying disorders. Immunoserological, microbiological, and pathological investigations are required to classify both MoC and MC as asymptomatic or symptomatic, and as essential or secondary. Asymptomatic individuals must be monitored over time for potential progression to overt clinical syndromes; similarly, those with essential forms require surveillance for the emergence of systemic diseases. Possible overlap with autoimmune conditions, particularly Sjögren’s disease, should always be considered.

Despite some shared features, MoCs and MCs represent distinct clinical entities. Accurate diagnosis relies primarily on cryoprecipitate analysis. MoCs are usually associated with thrombotic, non-inflammatory microangiopathy and lymphoproliferative disorders, whereas MCs are characterized by immune-complex–mediated leukocytoclastic vasculitis, complement consumption, and frequent association with viral infections, especially HCV and HBV. The introduction of new-generation antivirals in the last decade has markedly reduced the prevalence of virus-related MCs in more developed countries.

A harmonized nomenclature and standardized definitions for various cryoglobulinemia subsets, supported by careful clinical-immunological and pathological characterization, are essential to improve diagnostic accuracy, ensure interobserver consistency, and enable the development of evidence-based, mechanism-driven therapies for major cryoglobulinemic syndromes.

## Linked entities

- **Diseases:** cryoglobulinemia (MONDO:0005576)

## Full-text entities

- **Genes:** NOTCH4 (notch receptor 4) [NCBI Gene 4855] {aka INT3}, KRT20 (keratin 20) [NCBI Gene 54474] {aka CD20, CK-20, CK20, K20, KRT21}
- **Diseases:** immune dysregulation (OMIM:614878), clinical (MESH:D000075902), hepatocellular carcinoma (MESH:D006528), gangrene (MESH:D005734), Waldenstrom's macroglobulinemia (MESH:D008258), MGUS (MESH:D008998), coma (MESH:D003128), neuropathy (MESH:D009422), ischemic tissue damage (MESH:D017695), -cell (MESH:D002292), cryofibrinogenemia (MESH:C536218), Ray (MESH:C564523), hematological, rheumatic-autoimmune, and/or infectious disorders (MESH:D003141), lymphoid malignancies (MESH:D008223), purpura (MESH:D011693), xerostomia (MESH:D014987), B-cell lymphoid neoplasms (MESH:D016393), neuropathic pain (MESH:D009437), hematologic/lymphoproliferative disorders (MESH:D008232), renal disease (MESH:D007674), hepatic disease (MESH:D056486), paresthesias (MESH:D010292), motor neuropathy (MESH:D010523), Vasculitisor Type II/III (MESH:C536044), chronic hepatitis B virus (HBV) infection (MESH:D019694), Raynaud's phenomenon (MESH:D011928), B-NHL (MESH:D008228), systemic small vessel vasculitides (MESH:D056647), skin ulcers (MESH:D012883), infected (MESH:D007239), MPGN type I (MESH:D015432), MoC (MESH:D010265), immune (MESH:D007154), HCV or HBV infection (MESH:D006525), arthralgia (MESH:D018771), vascular injury (MESH:D057772), RF (MESH:D001171), weight loss (MESH:D015431), ulcers (MESH:D014456), Monoclonal and mixed cryoglobulinemia syndromes (MESH:C565141), renal involvement (MESH:C565423), leukocytoclastic vasculitis (MESH:C535509), glomerulonephritis (MESH:D005921), polyarthritis (MESH:D001168), vasculitic symptoms (MESH:D012816), HCV (MESH:D006526), RA (MESH:D001172), thrombotic (MESH:D013927), Hematological disorders (MESH:D006402), ataxia (MESH:D001259), Autoimmune systemic dis (MESH:D003643), viral infections (MESH:D014777), neurological manifestations (MESH:D009461), renal (MESH:D006030), B-cell lymphoproliferative diseases (MESH:D015448), Flares (MESH:D000067251), hematological, autoimmune, and/or infectious (MESH:D019337), Ig (MESH:D005922), vasculitic disorder (MESH:D009358), SLE (MESH:D008180)
- **Chemicals:** heparin (MESH:D006493), steroids (MESH:D013256), RTX (MESH:D000069283), entecavir (MESH:C413685), DAA (-), colchicine (MESH:D003078), cyclic citrullinated peptide (MESH:C487763), galactose (MESH:D005690), cyclophosphamide (MESH:D003520), methylprednisolone (MESH:D008775), methotrexate (MESH:D008727), bortezomib (MESH:D000069286), sialic acid (MESH:D019158), azathioprine (MESH:D001379), tenofovir (MESH:D000068698)
- **Species:** Human parvovirus B19 (no rank) [taxon 10798], human gammaherpesvirus 4 (Epstein Barr virus, no rank) [taxon 10376], Homo sapiens (human, species) [taxon 9606], Human immunodeficiency virus (species) [taxon 12721], Human immunodeficiency virus 1 (no rank) [taxon 11676], Hepatitis B virus (no rank) [taxon 10407], Severe acute respiratory syndrome coronavirus 2 (no rank) [taxon 2697049], hepatitis C virus [taxon 11103]

## Figures

4 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12964370/full.md

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Source: https://tomesphere.com/paper/PMC12964370