Race Disparities in Peptide Profiles of North American and Kenyan Wilms Tumor Specimens

Libes, Jaime; Seeley, Erin H.; Li, Ming; Axt, Jason R.; Pierce, Janene; Correa, Hernán; Newton, Mark; Hansen, Erik N.; Judd, Audra M.; McDonald, Hayes; Caprioli, Richard M.; Naranjo, Arlene; Huff, Vicki; O’Neill, James A.; Lovvorn, Harold N.

doi:10.1016/j.jamcollsurg.2013.12.044

Cited by 27 publications

(25 citation statements)

References 24 publications

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“…256 While we are not aware of any studies exploring the use of proteomics to characterize the relationship between race and allergic disease, peptide profiles and protein signatures that are specifically associated with several different cancer forms in patients of African ancestry have been identified. 257,258 Similarly, we can expect proteomics to play a future role in explaining racial disparities and identifying race-specific biomarkers associated with allergic disease. MicroRNAs (miRNAs) are small noncoding RNAs that act mainly as suppressors of gene expression at the posttranscriptional level, 259–261 which may act as key regulators of the development and activity of innate and adaptive immune systems and control inflammatory processes.…”

Section: Omics-based System Biology Approach To Atopic Disordersmentioning

confidence: 99%

Resolving the etiology of atopic disorders by using genetic analysis of racial ancestry

Gupta

Johansson

Bernstein

et al. 2016

Journal of Allergy and Clinical Immunology

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Atopic dermatitis (AD), food allergy (FA), allergic rhinitis (AR) and asthma are common atopic disorders of complex etiology. The frequently observed “atopic march” from early AD to asthma and/or AR later in life as well as the extensive comorbidity of atopic disorders, suggests common causal mechanisms in addition to distinct ones. Indeed, both disease-specific and shared genomic regions exist for atopic disorders. Their prevalence also varies among races; for example, AD and asthma have a higher prevalence in African-Americans when compared to European-Americans. Whether this disparity stems from true genetic or race-specific environmental risk factors or both is unknown. Thus far, the majority of the genetic studies on atopic diseases have utilized populations of European ancestry, limiting their generalizability. Large cohort initiatives and new analytic methods such as admixture mapping are currently being employed to address this knowledge gap. Here we discuss the unique and shared genetic risk factors for atopic disorders in the context of ancestry variations, and the promise of high-throughput “-omics” based systems biology approach in providing greater insight to deconstruct into their genetic and non-genetic etiologies. Future research will also focus on deep phenotyping and genotyping of diverse racial ancestry, gene-environment, and gene-gene interactions.

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Section: Omics-based System Biology Approach To Atopic Disordersmentioning

confidence: 99%

Resolving the etiology of atopic disorders by using genetic analysis of racial ancestry

Gupta

Johansson

Bernstein

et al. 2016

Journal of Allergy and Clinical Immunology

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“…The combined frequency of three genetic alterations fundamental to Wilms tumorigenesis, specifically WT1, CTNNB1, and WTX (i.e., AMER1 or FAM123B), has been estimated to occur in roughly one-third of WT, whereas aberrant expression of IGF2 has been shown to occur in 70% of WT specimens (Huff, 2011;Gadd et al, 2012). Furthermore, WT maintenance and disease progression are associated with the altered expression of multiple other genes, such as TP53, MYCN, CITED1, SIX2, TOP2A, and CRABP2 (Lovvorn et al, 2007;Schaub et al, 2007;Williams et al, 2011Williams et al, , 2015Murphy et al, 2012bMurphy et al, , 2014Libes et al, 2014a;Pierce et al, 2014). Specifically, mutations in TP53 and accumulation of its protein product, TP53, are a common finding in unfavorable histology (UH) WT and a notorious marker of treatment resistance (Lahoti et al, 1996;Sredni et al, 2001;Natrajan et al, 2007;Maschietto et al, 2014).…”

Section: Introductionmentioning

confidence: 99%

Genetic and chromosomal alterations in Kenyan Wilms Tumor

Lovvorn

Pierce

Libes

et al. 2015

Genes Chromosomes & Cancer

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Wilms tumor (WT) is the most common childhood kidney cancer worldwide and poses a cancer health disparity to black children of sub-Saharan African ancestry. Although overall survival from WT at 5 years exceeds 90% in developed countries, this pediatric cancer is alarmingly lethal in sub-Saharan Africa and specifically in Kenya (36% survival at 2 years). Although multiple barriers to adequate WT therapy contribute to this dismal outcome, we hypothesized that a uniquely aggressive and treatment-resistant biology compromises survival further. To explore the biologic composition of Kenyan WT (KWT), we completed a next generation sequencing analysis targeting 10 WT-associated genes and evaluated whole-genome copy number variation. The study cohort was comprised of 44 KWT patients and their specimens. Fourteen children are confirmed dead at 2 years and 11 remain lost to follow up despite multiple tracing attempts. TP53 was mutated most commonly in 11 KWT specimens (25%), CTNNB1 in 10 (23%), MYCN in 8 (18%), AMER1 in 5 (11%), WT1 and TOP2A in 4 (9%), and IGF2 in 3 (7%). Loss of heterozygosity (LOH) at 17p, which covers TP53, was detected in 18% of specimens examined. Copy number gain at 1q, a poor prognostic indicator of WT biology in developed countries, was detected in 32% of KWT analyzed, and 89% of these children are deceased. Similarly, LOH at 11q was detected in 32% of KWT, and 80% of these patients are deceased. From this genomic analysis, KWT biology appears uniquely aggressive and treatment-resistant.

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“…Peptides used to create these models can then be sequenced, their parent proteins identified, and queried for targetable moieties. (7) Once validated by an external tumor set, these data could be used to not only identify tumors with known outcomes, but also to potentially predict the likelihood of treatment failure or metastasis and thereby identify patients that would benefit from more intensive chemotherapy at the time of diagnosis.…”

Section: 4 Discussionmentioning

confidence: 99%

“…(8, 9) Prior work from our laboratory has delineated proteomic, tumor-specific differences between tumors from race groups that may explain the increased incidence and adverse WT behavior observed in minority groups. (7, 10, 11)…”

Section: 4 Discussionmentioning

confidence: 99%

Peptide spectra in Wilms tumor that associate with adverse outcomes

Murphy

Pierce

Seeley

et al. 2015

Journal of Surgical Research

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Background The 2013 Children’s Oncology Group (COG) blueprint for renal tumor research challenges investigators to develop new, risk-specific biological therapies for unfavorable histology and higher-risk Wilms tumor (WT) in an effort to close a persistent survival gap and to reduce treatment toxicities. As an initial response to this call from the COG, we used imaging mass spectrometry (IMS) to determine peptide profiles of WT associated with adverse outcomes. Materials and Methods We created a WT tissue microarray containing 2 mm punches of formalin-fixed, paraffin-embedded specimens archived from 48 sequentially treated WT patients at our institutions. IMS was performed to compare peptide spectra between three patient groups: unfavorable versus favorable histology, treatment success versus failure, and COG higher- versus lower-risk disease. Statistically significant peptide peaks differentiating groups were identified and incorporated into a predictive model using a Genetic algorithm. Results 131 peptide peaks were differentially expressed in unfavorable vs. favorable histology WT (p<0.05). 203 peaks differentiated treatment failure from success (p<0.05). 71 peaks differentiated COG higher-risk disease from the very-low, low, and standard risk groups (p<0.05). These peaks were used to develop predictive models that could differentiate between patient groups 98.49%, 94.46%, and 98.55% of the time respectively. Spectral patterns were internally cross-validated using a leave-20%-out model. Conclusions Peptide spectra can discriminate adverse behavior of WT. Following future external validation and refinement, these models could be used to predict WT behavior and to stratify intensity of chemotherapy regimens. Furthermore, peptides discovered in the model could be sequenced to identify potential risk-specific drug targets.

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Race Disparities in Peptide Profiles of North American and Kenyan Wilms Tumor Specimens

Cited by 27 publications

References 24 publications

Resolving the etiology of atopic disorders by using genetic analysis of racial ancestry

Resolving the etiology of atopic disorders by using genetic analysis of racial ancestry

Genetic and chromosomal alterations in Kenyan Wilms Tumor

Peptide spectra in Wilms tumor that associate with adverse outcomes

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