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Acute Monoclonal Gammopathy in Severe COVID-19 - PMC

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18/10/23, 11:52 “Acute” monoclonal gammopathy in severe COVID-19 - PMC

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Hematol Transfus Cell Ther. 2020 Jul-Sep; 42(3): 218–220. PMCID: PMC7280116
Published online 2020 Jun 9. doi: 10.1016/j.htct.2020.05.002 PMID: 32546369

“Acute” monoclonal gammopathy in severe COVID-19


Natale Vazzana,⁎ Silvia Ognibene, and Francesco Dipaola

Dear Editor,

Laboratory findings in severe coronavirus disease (COVID)-19 may include lymphopenia, elevated
D-dimer, lactate dehydrogenase (LDH), C-reactive protein (CRP), and ferritin.1 Several quantitative
and functional abnormalities in lymphocyte populations have been reported in patients with
SARS-CoV-2 infection, with evidence of depletion of cytotoxic T-lymphocytes and natural killer
cells.2 Lymphopenia has been identified as a prognostic marker for poor outcomes as it could be
in correlation with cytokine storm.1 Though numerically depleted, circulating reactive lymphocytes
were detectable in a consistent proportion of patients, some of them with a lymphoplasmacytic
phenotype.3, 4 Whether this cell population is related to polyclonal or monoclonal hypergamma‐
globulinemia is still unknown.

During SARS-CoV-2 outbreak in our region, we observed the case of an 80-year old man with se‐
vere COVID-19 and evidence of a transient monoclonal gamma-globulin spike (Figure 1, case 1).
He had no previous evidence of monoclonal gammopathy and his serum protein electrophoresis
(SPEP) was normal 9-month before. He was admitted to our COVID ward because of fever, malaise
and increasing dyspnea. His nasopharyngeal swab was positive for SARS-CoV-2 RNA. Chest high-
resolution computed tomography (HRCT) revealed bilateral ground-glass opacities and interlobu‐
lar septal thickening. Treatment with hydroxychloroquine, lopinavir/ritonavir and antibiotics was
given, with no significant improvement. At D9 blood tests revealed lymphopenia (740 μL−1), in‐
creased LDH (809 UI/L), ferritin (1879 ng/mL), and CRP (17.6 mg/dL). Prothrombin time was
slightly prolonged (14.1 s), whereas platelet count (489 × 109 L–1) and fibrinogen (>900 mg/dL)
were increased. A monoclonal band was found on SPEP and it was characterized as IgG-lambda by
immunofixation. Steroid treatment was added, and non-invasive ventilation was necessary from
D17 to D21, when initial improvement in his respiratory status was observed. A repeated SPEP
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18/10/23, 11:52 “Acute” monoclonal gammopathy in severe COVID-19 - PMC

showed a significant decrease in M-protein, in parallel with reduction of inflammatory biomarkers


and lymphocyte reconstitution. He then developed sepsis sustained by P. aeruginosa, successfully
treated with piperacillin/tazobactam. His condition gradually improved and supplemental oxygen
was stopped at D52. He was still in hospital for respiratory rehabilitation at time of manuscript
preparation.

Figure 1

Serum protein electrophoresis, laboratory and clinical course of case 1 and case 2. Abbreviations: HCQ+LPV/r, hy‐
droxychloroquine plus lopinavir/ritonavir, HCQ + DRV/c, hydroxychloroquine plus darunavir/cobicistat; VM,
Venturi mask.

Even though SPEP was not systematically incorporated for COVID-19 evaluation at our
Department, we observed similar findings in another 80-years old patient with COVID-19 related
pneumonia who had a severe course of disease (Figure 1, case 2). He was admitted to our COVID
Unit because of fever and non-productive cough. Bilateral patchy consolidations were seen on
HRCT. His medical history included arterial hypertension, hypothyroidism and previous carotid
thromboendarterectomy. No monoclonal spikes were observed in a past SPEP. Treatment with hy‐
droxychloroquine, darunavir/cobicistat and antibiotics was given but his respiratory status con‐
tinued to deteriorate. High-flow oxygen was administered through a non-rebreather face mask

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18/10/23, 11:52 “Acute” monoclonal gammopathy in severe COVID-19 - PMC

and steroid treatment was started. At D8, there was severe lymphopenia (250 μL−1), increased
LDH (529 UI/L), ferritin (959 ng/mL), fibrinogen (797 mg/dL), and CRP (17.9 mg/dL). Platelet
count and prothrombin time were within the normal range, whereas D-dimer was markedly in‐
creased (14,794 ng/mL) without clinical or echographic evidence of venous thromboembolism.
An IgG-kappa monoclonal band was found in his SPEP. The subsequent clinical course was favor‐
able, allowing a gradual reduction in oxygen therapy and steroid tapering. The monoclonal com‐
ponent was significantly decreased in a repeated SPEP at D26, together with normalization of lym‐
phocyte count, ferritin and CRP. Supplemental oxygen was discontinued at D17 and the patient
was discharged after 13 days.

Monoclonal gammopathy results from clonal proliferation of plasma cells or antibody secreting B-
cells, producing large amounts of homogenous immunoglobulin or light chain fragments. An
“acute” or transitory monoclonal spike has been reported in association with a spectrum of acute
and chronic inflammatory illnesses, including viral infections. In severe COVID-19 there is a mas‐
sive release of IL-6, which is associated with adverse clinical outcomes.5 IL-6 has been recognized
as a crucial growth factor for B-cell differentiation and terminal maturation into plasma cells,6
thus providing a mechanistic between severe COVID-19 and gamma-globulin peak production.
Lymphocyte depletion could also result in a loss of regulatory T cell-mediated suppression of
aberrant B-cell clones, with consequent dysregulated antibody production, which often regress af‐
ter immune-restoration, as observed in our patients. It should be noted that both cases were
recorded in elderly subjects, in which underlying aging-related subclinical plasma cells disorders
are more frequent and could represent a prerequisite for dysregulated antibody production dur‐
ing SARS-CoV-2 infection.

In conclusion, based on these data it could be hypothesized that the presence of a monoclonal
spike during the inflammatory phase could reflect the degree of immune hyperactivation in pa‐
tients with severe COVID-19. Further studies are needed to evaluate its frequency, long-term evo‐
lution and prognostic role in this clinical setting.

Contributorship

All authors managed the patient. NV was responsible for writing, NV and SO for the figure and FD
for the literature search.

Conflicts of interest

The authors declare no conflicts of interest.

References

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https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7280116/ 4/4

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