Light chain multiple myeloma, clinic features, responses to therapy and survival in a long-term study

Zhang, Jia-Jia; Sun, Wei; Huang, Zhongxia; Chen, Shi-lun; Zhong, Yuanyuan; Hu, Ying; An, Na; Shen, Man; Li, Xin

doi:10.1186/1477-7819-12-234

Cited by 24 publications

(38 citation statements)

References 13 publications

(10 reference statements)

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“…This could possibly indicate that disease progression could be enumerated by the number of CTAs expressed in this panel and could be used to re-evaluate patients if disease progression is suspected. Only a small group of patients represented either the IgA or light chain disease subtypes, both of which are associated with a worse overall survival [33,34]. While no significant associations could be found regarding the IgA grouping, due to low numbers, the light chain diseased patients all grouped together expressing 5-6 CTAs and demonstrated advanced clinical symptoms.…”

Section: Discussionmentioning

confidence: 93%

“…The characteristics of the plasma cells, including their presence in the PB, proliferation status and their abnormal nuclear staining are additional independent prognostic factors that can be considered. Circulating plasma cells, which is indicative of more aggressive disease [33,34] were only observed in 9 patients, 78% of whom presented with stage III disease. However, this subgrouping showed no specific CTA expression pattern (in number or specific gene).…”

Section: Links Between the Number Of Ctas Expressed And Disease Charamentioning

confidence: 99%

“…This association was further strengthened by the increase in the number of CTAs expressed by two AMM patients who progressed to MM within 12 months, both showing no CTA expression at initial diagnosis and 3 (stage II) and 6 (stage III) genes, respectively at follow up. With regards to disease subtype, light chain MM disease is known to offer a worse prognosis [32,33], with rapid kidney failure. While we only had 5 patients in this grouping at diagnosis, all presented with advanced disease (stage III, 3-4 CRAB symptoms) and correspondingly expressed 5-6 CTAs (Figure 2).…”

Section: Links Between the Number Of Ctas Expressed And Disease Charamentioning

confidence: 99%

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Cancer/Testis Antigen Expression Panel Incorporating MAGEC1 and BAGE2 Predicts Multiple Myeloma Disease Stage and Severity

Shires

Teuchert²,

Wienand³

et al. 2016

J Hematol Thrombo Dis

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To provide a single molecular assay that could be used to easily stage Multiple Myeloma patients at diagnosis, we investigated the association between the simultaneous expression of 7 Multiple Myeloma-associated Cancer/Testis Antigens and biochemical parameters that are currently used for disease staging. We analysed the mRNA expression of MAGEC1, MAGEA3/A6, BAGE2, PRAME, NYESO1, SSX2 and PAGE by qualitative reverse transcription PCR using RNA extracted from diagnostic bone marrow samples from 39 patients covering the Multiple Myeloma disease continuum and compared this to levels of key biochemical parameters at diagnosis. We found that the Cancer/Testis Antigen panel was expressed in a specific order that was specifically associated with the severity of disease. This allowed the Cancer/Testis Antigens expression profile to successfully place the patient clearly into either stage I or stage III of the disease, with further sub-stratification in the stage III grouping. In addition, we putatively identified MAGEC1 expression as a confirmatory diagnostic marker for symptomatic Multiple Myeloma and clearly associated BAGE2 expression exclusively with stage III disease. We also demonstrated the novel finding of PAGE expression in Multiple Myeloma, with an association with more advanced disease. We suggest that this particular molecular Cancer/Testis Antigen panel can be used at diagnosis as a single test to clearly stage patients.

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Section: Discussionmentioning

confidence: 93%

Section: Links Between the Number Of Ctas Expressed And Disease Charamentioning

confidence: 99%

Section: Links Between the Number Of Ctas Expressed And Disease Charamentioning

confidence: 99%

See 1 more Smart Citation

Cancer/Testis Antigen Expression Panel Incorporating MAGEC1 and BAGE2 Predicts Multiple Myeloma Disease Stage and Severity

Shires

Teuchert²,

Wienand³

et al. 2016

J Hematol Thrombo Dis

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“…В опубликованных работах, посвященных проблемам ММ, практически не обсуждалась локализация болей у пациентов, указывалась только общая частота болевого синдрома [19][20][21]. В нашем исследовании наиболее часто встречалась множественная локализация болей (38,9%), следовательно, наличие алгического синдрома множе-ственной локализации может служить ранним признаком миеломной болезни и должно побуждать врачей к ее диа-гностическому поиску.…”

Section: Discussionunclassified

Clinical characteristics of pain syndrome in patients with multiple myeloma

Stamo¹,

Grigorieva²

2016

Z. nevrol. psikhiatr. im. S.S. Korsakova

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“…Production of this aberrant Ig results in several of the complications associated with MM such as renal dysfunction, neuropathy, and hyperviscosity syndrome 23 . However, in approximately 15–20% of patients the abnormal plasma cells secrete only monoclonal free light chains, and in approximately 2–3% of cases these cells secrete no monoclonal protein at all, resulting in the so-called non-secretory myeloma 45 . Myeloma cell growth in the bone marrow and the resultant cytokines produced by these transformed cells lead to the classic symptoms of active MM: osteolytic bone lesions, hypercalcemia, and anemia 6 .…”

Section: Multiple Myelomamentioning

confidence: 99%

The challenges of checkpoint inhibition in the treatment of multiple myeloma

Paul

Kang

Zheng

et al. 2018

Cellular Immunology

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Despite significant improvements in the overall survival of patients with multiple myeloma (MM) over the past 15 years, the disease remains incurable. Treatment options are limited for patients who have relapsed or are refractory to immunomodulatory drugs (IMiDs), proteasome inhibitors, and monoclonal antibodies. In these patients, immunotherapies such as checkpoint inhibitors, oncolytic vaccines, and chimeric antigen receptor (CAR) T cells provide a potentially effective alternative treatment. While checkpoint inhibitors are effective in prolonging overall survival in some patients with advanced solid cancers and Hodgkin lymphoma, they have not demonstrated significant anti-myeloma activities as a single agent in MM. In fact the combination of checkpoint inhibitors with IMiDs was recently found to increase the risk of death in myeloma patients. These challenges highlight the need for a better understanding of immune dysregulation in myeloma patients, and the mechanisms of action of- and resistance to- checkpoint inhibitors. In this review, we summarize immune dysfunction in patients with MM, and review the preclinical and clinical data regarding checkpoint inhibitors in myeloma. We conclude by proposing strategies to improve the efficacy and safety of checkpoint inhibitors in this population.

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Light chain multiple myeloma, clinic features, responses to therapy and survival in a long-term study

Cited by 24 publications

References 13 publications

Cancer/Testis Antigen Expression Panel Incorporating MAGEC1 and BAGE2 Predicts Multiple Myeloma Disease Stage and Severity

Cancer/Testis Antigen Expression Panel Incorporating MAGEC1 and BAGE2 Predicts Multiple Myeloma Disease Stage and Severity

Clinical characteristics of pain syndrome in patients with multiple myeloma

The challenges of checkpoint inhibition in the treatment of multiple myeloma

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