Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
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Target Concepts:
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Query: UNIPROT:P05231 (
interleukin-6
)
23,907
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
A possible autocrine effect of
interleukin-6
(
IL-6
) on the growth and differentiation of the tumor cells of 55 B-cell lymphomas was examined.
Interleukin-6
was detected in a few types of B-cell lymphomas, including polymorphic immunocytoma (PI),
small lymphocytic lymphoma
(
SLL
), and immunoblastic lymphoma (IBL) with or without plasmacytoid differentiation. In PI and in IBL with plasmacytoid differentiation (IBL-P),
IL-6
was detected only in immunoglobulin-containing plasmacytoid cells, and it was absent from most proliferating (Ki-67/PCNA-positive) lymphoma cells. In
SLL
,
IL-6
was not observed in lymphoplasmacytoid cells; instead,
IL-6
was observed in transformed (Ki-67/PCNA-positive) tumor cells in proliferation centers. The lymphoplasmacytoid cells in
SLL
exhibited a phenotype (
IL-6
/glutathione-S-transferase-pi [GST-pi]-negative), different from that of normal plasma cells (
IL-6
-negative/GST-pi-positive) and from the plasmacytoid cells (
IL-6
/GST-pi-positive) in PI and IBL-P. In IBL without obvious plasmacytoid differentiation,
IL-6
was detected in most tumor cells that were highly proliferative (Ki-67/PCNA-positive). In this study,
IL-6
was undetectable in most lymphomas related to follicular centers, in lymphoblastic lymphoma, in small noncleaved cell lymphomas of the Burkitt and non-Burkitt types, and in diffuse large cell lymphoma. This finding is compatible with a previous finding that
IL-6
mRNA was absent from follicular center cells in reactive lymphoid tissues. The functions of
IL-6
in these lymphomas may be quite diverse. It appears that
IL-6
, as an autocrine factor, is responsible for the plasmacytoid differentiation of lymphoma cells in IP and some IBL (IBL-P). The differentiation of lymphoplasmacytoid lymphoma cells in
SLL
, however, may not be mediated by an autocrine
IL-6
mechanism.
Interleukin-6
may provide a growth signal, rather than acting as a differentiation factor, for some IBL cells and for some transformed tumor cells in proliferation centers in
SLL
.
...
PMID:Functional heterogeneity and pathogenic significance of interleukin-6 in B-cell lymphomas. 141 84
Cardiac toxicity as a side effect of chemotherapeutic agents has been well reported in the literature. Cardiac toxicity secondary to alemtuzumab has been reported, presenting as congestive heart failure and arrhythmias. Here we report a case of acute myocardial dysfunction after administration of a test dose of alemtuzumab. Our patient was a 66-year-old man with a history of
small lymphocytic lymphoma
/chronic lymphocytic lymphoma who received a test dose of alemtuzumab. Twenty minutes post administration, the patient developed nausea, vomiting, rigors, and tachycardia. Electrocardiography (ECG) showed acute ST-segment elevations in contiguous leads V2-V6, I, and AVL with no associated chest pain. Bedside echocardiogram showed akinesis of the anterior septum, apex, distal anterior wall, and decreased left ventricular ejection fraction. Cardiac catheterization showed non-critical occlusive disease and no intervention was undertaken. Post-catheterization ECG revealed resolution of ST segment elevations, TWI in V4-V6, and prolongation of corrected QT. Repeat echocardiogram 10 days after the event demonstrated no improvement in wall motion or ejection fraction. We discuss the possible mechanisms causing ST-elevations and acute myocardial dysfunction after treatment with alemtuzumab. <
Learning objective:
Alemtuzumab can cause acute myocardial dysfunction after administration of a test dose. Considering that this is a serious adverse effect, detailed cardiac evaluation and a high level of caution are recommended before administration of alemtuzumab. While no clear etiology could be identified for this side effect, excessive and acute cytokine release triggered by alemtuzumab administration is a possible explanation. This could be potentially attenuated by using anti-
interleukin-6
or tumor necrosis factor inhibitors.>.
...
PMID:Alemtuzumab induced ST-segment elevation and acute myocardial dysfunction. 3053 36
