A Polymorphism in the Complement Component<i>C1qA</i>Correlates with Prolonged Response Following Rituximab Therapy of Follicular Lymphoma

Racila, Emilian; Link, Brian K.; Weng, Wen‐Kai; Witzig, Thomas E.; Ansell, Stephen M.; Maurer, Mathew S.; Huang, Jian; Dahle, Christopher E.; Halwani, Ahmad; Levy, Ronald; Weiner, George J.

doi:10.1158/1078-0432.ccr-08-0745

Cited by 136 publications

(92 citation statements)

References 52 publications

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“…Similarly, several studies, although small, have implicated C1q in the emergence of SLE, as several genetic variants located in the C1q region seem to associate with this disease [18][19][20][21][22]. In addition, two small studies indicated an effect of genetic variants of C1q on the progression of cancer and the efficacy of rituximab treatment for lymphoma [23,24].…”

Section: Introductionmentioning

confidence: 99%

Genetic variants in the region of the C1q genes are associated with rheumatoid arthritis

Trouw

Daha

Kurreeman

et al. 2013

Clinical and Experimental Immunology

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SummaryRodent models for arthritis implicate a role for complement in disease development and progression. In humans, complement deposition has been observed in inflamed synovia of rheumatoid arthritis (RA) patients. In this study we analysed whether genetic variants of complement component C1q predispose to RA. We genotyped single nucleotide polymorphisms (SNPs) in and around the C1q genes, C1qA, C1qB and C1qC, in a Dutch set of 845 RA cases and 1046 controls. Replication was sought in a sample set from North America (868 cases/1193 controls), and a meta-analysis was performed in a combined samples set of 8000 cases and 23 262 controls of European descent. We determined C1q serum levels in relation to C1q genotypes. In the discovery phase, five of the 13 SNPs tested in the C1q genes showed a significant association with RA. Additional analysis of the genomic area around the C1q genes revealed that the strongest associating SNPs were confined to the C1q locus. Within the C1q locus we observed no additional signal independent of the strongest associating SNP, rs292001 [odds ratio (OR) = 0·72 (0·58-0·88), P = 0·0006]. The variants of this SNP were associated with different C1q serum levels in healthy controls (P = 0·006). Interestingly, this SNP was also associated significantly in genome-wide association studies (GWAS) from the North American Rheumatoid Arthritis Consortium study, confirming the association with RA [OR = 0·83 (0·69-1·00), P = 0·043]. Combined analysis, including integrated data from six GWAS studies, provides support for the genetic association. Genetic variants in C1q are correlated with C1q levels and may be a risk for the development of RA.

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Section: Introductionmentioning

confidence: 99%

Genetic variants in the region of the C1q genes are associated with rheumatoid arthritis

Trouw

Daha

Kurreeman

et al. 2013

Clinical and Experimental Immunology

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“…Under our staged design, assuming a co-dominant model, a minor allele frequency of 0.44 and a joint analysis a level of 0.05, we had 97% power to detect an HR of 1.3. Power was not as good for the dominant (AG/GG vs AA) model, where we had 72% power to detect the same effect; however, power is 100% for HRs above 1.5, leaving our study more than adequately powered to detect a dominant effect similar to the one reported by Racila et al (2008). On the basis of our earlier finding that C1QA expression was associated with survival in ER-negative tumours, we stratified our sample by ER status.…”

Section: Discussionmentioning

confidence: 94%

“…There are seven single nucleotide polymorphisms (SNPs) catalogued for C1QA on the NCBI database, of which there is only one common SNP (minor allele frequency 45%) located in an exon rs172378 is a synonymous SNP characterised by a G for A substitution at position 361 (A361G). This SNP has been previously reported as being associated with breast cancer metastasis to sites linked to hematogenous spread of disease (Racila et al, 2006) and with drug response in follicular lymphoma (Racila et al, 2008). In a set of 63 patients with localised breast tumours and 38 patients with metastasis, Racila et al (2006) reported a decreased time to metastasis for G homozygote or heterozygote individuals compared with the common AA homozygote (hazard ratio, 95% CI: 2.4, 1.1 -4.1), even after adjustment for positive lymph nodes, oestrogen and progesterone receptors status.…”

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confidence: 90%

Common germ-line polymorphism of C1QA and breast cancer survival

et al. 2010

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BACKGROUND: A synonymous single nucleotide polymorphism (SNP) rs172378 (A4G, GlyÀ4Gly) in the complement component C1QA has been proposed to be associated with distant breast cancer metastasis. We previously reported overexpression of this gene to be significantly associated with better prognosis in oestrogen-receptor-negative tumours. The purpose of this study was to investigate the association of rs172378 with expression of C1QA and breast cancer survival. METHODS: We analysed the gene expression pattern of rs172378 in normal and tumour tissue samples, and further explored its involvement in relation to mortality in 2270 women with breast cancer participating in Studies of Epidemiology and Risk factors in Cancer Heredity, a population-based case -control study. RESULTS: We found that although rs172378 showed differential allelic expression significantly different between normal (preferentially expressing the G allele) and tumour tissue samples (preferentially expressing the A allele), there was no significant difference in survival by rs172378 genotype (per allele hazard ratio (HR) 1.02, 95% CI: 0.88 -1.19, P ¼ 0.78 for all-cause mortality; HR 1.03, 95% CI: 0.87 -1.22, P ¼ 0.72 for breast-cancer-specific mortality). CONCLUSION: Our study results show that rs172378 is linked to a cis-regulatory element affecting gene expression and that allelic preferential expression is altered in tumour samples, but do not support an association between genetic variation in C1QA and breast cancer survival.

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“…Clinical samples have also been used to establish correlations between the genetic makeup of the patient and response to rituximab using normal cells to study genetic polymorphisms. 15,16 Tumor samples may also be used to analyse expression profiles and establish correlations with response to mAbs. 17 …”

Section: Models Used To Understand Rituximab Cytotoxicity or Resistanmentioning

confidence: 99%

“…Homozygous A subjects achieved complete response at a higher rate than heterozygous or homozygous G subjects. 16 Tumor-related factors that are involved in resistance to rituximab include alteration in CD20 and lipids raft domain and regulation in signaling and mitochrondrial pathways (Fig. 2).…”

Section: Parameters Correlated With Rituximab Activity and Resistancementioning

confidence: 99%

Understanding and circumventing resistance to anticancer monoclonal antibodies

Reslan

Dalle

Dumontet

2009

mAbs

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With the widespread use of therapeutic monoclonal antibodies in the treatment of patients with cancer, resistance to these agents has become a major issue. Preclinical models of drug action or resistance have contributed to unravel the main mechanisms of resistance, involving both tumor-associated and host related factors. However our understanding of how a monoclonal antibody destroys cancer cells in a patient and why it one day stops being effective are still far from being complete. This review focuses on the available data on mechanisms of action and resistance to rituximab and includes some additional information for other monoclonal antibodies. Innovative approaches designed to overcome resistance, such as combination immunotherapy, costimulation with cytokines or growth factors are presented.

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A Polymorphism in the Complement ComponentC1qACorrelates with Prolonged Response Following Rituximab Therapy of Follicular Lymphoma

Cited by 136 publications

References 52 publications

Genetic variants in the region of the C1q genes are associated with rheumatoid arthritis

Genetic variants in the region of the C1q genes are associated with rheumatoid arthritis

Common germ-line polymorphism of C1QA and breast cancer survival

Understanding and circumventing resistance to anticancer monoclonal antibodies

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