With the increase in technological capabilities for measuring biological molecules, there is a greater trend to conduct non-biased, discovery-driven studies that collect information on hundreds of molecules in a single study. The hope is that novel findings can be detected within these large datasets. For protein analysis, these non-biased studies are particularly challenging as no technology is presently capable of providing a view of the entire proteome. The ability of non-biased studies to accurately detect specific differences within the proteomes of samples obtained from differentially treated individuals must be conclusively demonstrated before investigators will routinely adopt these methods as part of their experimental protocols. This need is especially true for clinical and epidemiological studies in which limited amounts of samples are available

Veenstra, Timothy D.

English

Digital Commons

Cedarville University DigitalCommons@Cedarville Pharmaceutical Sciences Faculty Publications Department of Pharmaceutical Sciences 6-5-2009 Using a Global Proteomic Approach to Identify Proteins Affected by Estrogen Therapy Timothy D. Veenstra Cedarville University, tveenstra@cedarville.edu Follow this and additional works at: https://digitalcommons.cedarville.edu/pharmaceutical_sciences_publications  Part of the Pharmacy and Pharmaceutical Sciences Commons Recommended Citation Veenstra, Timothy D., "Using a Global Proteomic Approach to Identify Proteins Affected by Estrogen Therapy" (2009). Pharmaceutical Sciences Faculty Publications. 293. https://digitalcommons.cedarville.edu/pharmaceutical_sciences_publications/293 This Article is brought to you for free and open access by DigitalCommons@Cedarville, a service of the Centennial Library. It has been accepted for inclusion in Pharmaceutical Sciences Faculty Publications by an authorized administrator of DigitalCommons@Cedarville. For more information, please contact digitalcommons@cedarville.edu. Genome Medicine 2009, 1:58CommentaryUsing a global proteomic approach to identify proteins affected by estrogentherapyTimothy D VeenstraAddress: Laboratory of Proteomics and Analytical Technologies, Advanced Technology Program, SAIC-Frederick Inc., National CancerInstitute at Frederick, Frederick, MD 21702, USA. Email: veenstra@ncifcrf.govAbstractWith the increase in technological capabilities for measuring biological molecules, there is agreater trend to conduct non-biased, discovery-driven studies that collect information onhundreds of molecules in a single study. The hope is that novel findings can be detected withinthese large datasets. For protein analysis, these non-biased studies are particularly challenging asno technology is presently capable of providing a view of the entire proteome. The ability of non-biased studies to accurately detect specific differences within the proteomes of samples obtainedfrom differentially treated individuals must be conclusively demonstrated before investigators willroutinely adopt these methods as part of their experimental protocols. This need is especiallytrue for clinical and epidemiological studies in which limited amounts of samples are available.Published: 5 June 2009Genome Medicine 2009, 1:58 (doi:10.1186/gm58)The electronic version of this article is the complete one and can befound online at http://genomemedicine.com/content/1/6/58© 2009 BioMed Central Ltd Conjugated equine estrogens (CEE) have been widelyadministered for the relief of menopausal symptoms [1].While there are obvious benefits to women suffering frommenopausal symptoms, estrogens are also known to exertharmful effects. For instance, the evidence linking estrogenmetabolite levels and cancers of the reproductive systemcontinues to grow [2]. Scientists are also studying the effectsof estrogen metabolites in different racial populations. Withthis information, physicians now are faced with wonderingwhich of their patients should have CEE administered. Theshort-term benefits need to be carefully weighed against anypossible long-term detriments.In 2003, the Women’s Health Initiative (WHI) reported thatwomen being administered CEE plus progesterone had anincreased number of cardiovascular events compared tothose given a placebo [3]. Unfortunately, confusion aboutthe benefits of hormone replacement therapy (HRT) wasintroduced with the 2004 WHI estrogen-only trial thatshowed no increase in such cardiovascular events. Althoughthis study did not provide a conclusive answer, it did suggestthat women aged 50 to 59 years who received estrogentherapy enjoyed lower rates of heart disease [4]. A recentstudy, entitled the WHI Coronary-Artery Calcium Study(WHI-CACS), examined the effects of estrogen on coronary-artery calcification in women between the ages of 50 and 59who were enrolled in the CEE trial [5]. The results of thisstudy showed that women receiving estrogen had lesscoronary-artery calcification compared to the control groupreceiving a placebo.Estrogen therapy is known to affect large numbers ofproteins and metabolites, beyond those related to cardio-vascular events. Low- and high-density lipoproteins, tri-glycerides, insulin, insulin-like growth factors, glucose andC-reactive protein are just a few of the molecules whoselevels have been shown to be affected by estrogen adminis-tration. Considering the wide range of effects that estrogenexerts, there are undoubtedly many as yet undiscoveredmolecules and functional pathways that are affected byestrogen treatment. In the recent article published inGenome Medicine entitled ‘Application of serum proteomicsto the Women’s Health Initiative conjugated estrogen equineestrogens trial reveals a multitude of effects relevant toclinical findings’, Katayama et al. [6] sought to discovernovel proteomic changes affected by CEE and also validatethe efficacy of using a global proteomic strategy for findingthese differences. This group used a method termed intactprotein analysis system (IPAS) to compare protein levels inserum samples collected from women prior to initiation ofCEE treatment and one year after initiation of treatment.Five separate analyses were conducted using samplesacquired from 50 women. The samples were prepared bypooling equal-volume aliquots from groups of ten women.The IPAS system utilizes two dimensions of chromatography(anion exchange followed by reversed-phase) to fractionateintact proteins. Aliquots collected from the reversed-phasecolumn are tryptically digested and the proteins are identi-fied and quantified using high-throughput mass spectro-metry (MS). Prior to their chromatographic separation, theproteins from the CEE-treated and control group weredifferentially isotopically labeled to allow their relativeabundances to be measured via the MS measurements. All ofthe serum samples were also subjected to high-abundantprotein depletion, eliminating such proteins as albumin andimmunoglobulins from the analysis. The combination ofhigh-abundant protein removal and extensive fractionationpermitted proteins across seven orders of magnitude ofabundance to be measured.A total of 611 proteins were quantified between the serumsamples acquired pre- and one-year post-CEE treatment. Astatistically significant difference in the abundance of 116proteins was observed between the two comparativesamples. Of these, 64 proteins had a false discovery rate(FDR) less than 0.5 relative to all of the quantified proteins.Classification of these proteins into networks revealed fivesignificant functional processes that were affected by CEEtreatment: blood coagulation, kallikrein-kinin system, celladhesion-platelet-endothelium-leukocyte interactions, comple-ment system, and ossification. Comparison of these 64proteins to previous findings yielded 13 (>20%) that hadbeen reported in the literature to have an association withestrogen therapy. The remaining 41 proteins where noassociation with estrogen therapy had been previouslyreported were associated with functions such as bloodcoagulation, ossification, cell growth, blood pressure main-tenance, blood vessel morphogenesis, and angiogenesis. Toconfirm the IPAS results, enzyme-linked immunosorbentassays (ELISAs) were carried out on 13 of the proteins usingboth non-pooled samples that were part of the original IPASstudy and an independent sample set. In both validationtests, the correlation between the results obtained fromthese two methods was >0.83.This manuscript provides an excellent demonstration of thevalue of global comparative proteomic studies. Using a non-biased method, Katayama et al. were able to correlate theirresults with a number of findings that had previously beenreported to be associated with CEE. For example, CEE hasbeen associated with a reduction in hip fractures. Theauthors were able to discover several proteins related toossification and osteogenesis that had increased abundancesin samples obtained from women that had been adminis-tered CEE. They were also able to show changes in severalproteins that play roles in circulatory processes such ascoagulation, angiogenesis, and blood pressure regulation.These results may be connected to the previously mentionedbenefits of lower heart disease rates.There is a misconception related to the value of the infor-mation to be gleaned from global proteomic studies asillustrated by Katayama et al. Many scientists that areunfamiliar with the technology anticipate that a globalcomparison provides a ‘neat little package’ of proteins whoseabundance is affected by a particular stimulus. Unfortu-nately, many investigators are exasperated when the datathey receive back is a long list of proteins with a largenumber of them showing a change in abundance. Ofteninvestigators find that the number of observed differencesoverwhelms their ability to decide which direction to follow.Katayama et al. have done an excellent job demonstratingthe efficacy of turning a list of proteins into meaningfulconclusions and further hypotheses. By grouping theproteins that showed a significant change in abundance theywere able to uncover functional pathways that were affectedby CEE treatment. These findings can now be used to inter-rogate specific proteins in order to gather a greater depth ofinformation concerning the effect of CEE on a physiologicalfunction. In this study, a number of CEE-associatedfunctions were uncovered, some previously shown and somenovel. Following up on these non-biased results requiresselection of those functions that are most critical from apublic health view. This decision, while highly subjective,needs to carefully consider the quality of the data obtainedin the global comparative study and the relative functionalimportance of each protein pathway. For example, in thesearch for a cancer biomarker, considerable effort would notbe exerted to further study acute phase response proteins,although many of these would probably be detected ashaving higher abundances in samples taken from cancer-affected individuals.What this study has illustrated is the utility of globalcomparative proteomic analyses for identifying changes inprotein abundances within clinical samples obtained fromdifferent groups of individuals. The affected proteins wereadequately validated using an orthogonal method andindependent sample set. While this study is not the first touse a non-biased global approach to discover proteins andmolecules that change as a result of an external pertur-bation, health scientists and institutions are still reluctant toutilize technologies (such as the type used in this study) toconduct investigative research. While such global proteomicstudies can be time consuming, taking months to complete,the richness of information obtainable more than makes uphttp://genomemedicine.com/content/1/6/58 Genome Medicine 2009, Volume 1, Issue 6, Article 58 Veenstra 58.2Genome Medicine 2009, 1:58for the effort spent. In this CEE study, five functional groupsof proteins were discovered to be perturbed, using the samedata set. This wealth of information provides large numbersof hypotheses to be tested. Non-biased global studies, asillustrated in this manuscript, are a very efficient route todiscovering novel effects of perturbations to biologicsystems.AbbreviationsCEE, conjugated equine estrogens; ELISA, enzyme-linkedimmunosorbent assay; FDR, false discovery rate; HRT,hormone replacement therapy; IPAS, intact protein analysissystem; MS, mass spectrometry; WHI, Women’s HealthInitiative; WHI-CACS, WHI Coronary-Artery Calcium Study.Competing interestsThe author declares that he has no competing interests.AcknowledgementsThis project has been funded in whole or in part with federal funds fromthe National Cancer Institute, National Institutes of Health, under Con-tract HHSN261200800001E. The content of this publication does notnecessarily reflect the views or policies of the Department of Health andHuman Services, nor does mention of trade names, commercial products,or organizations imply endorsement by the US Government.References1. Nelson HD: Commonly used types of postmenopausal estrogen fortreatment of hot flashes: scientific review. JAMA 2004, 291:1610-1620.2. Eliassen AH, Hankinson SE: Endogenous hormone levels and risk ofbreast, endometrial and ovarian cancers: prospective studies. AdvExp Med Biol 2008, 630:148-165.3. Manson JE, Hsia J, Johnson KC, Rossouw JE, Assaf AR, Lasser NL,Trevisan M, Black HR, Heckbert SR, Detrano R, Strickland OL,Wong ND, Crouse JR, Stein E, Cushman M; Women’s Health Initia-tive Investigators: Estrogen plus progestin and the risk of coronaryheart disease. N Engl J Med 2003, 349:523-534.4. Anderson GL, Limacher M, Assaf AR, Bassford T, Beresford SA,Black H, Bonds D, Brunner R, Brzyski R, Caan B, Chlebowski R,Curb D, Gass M, Hays J, Heiss G, Hendrix S, Howard BV, Hsia J,Hubbell A, Jackson R, Johnson KC, Judd H, Kotchen JM, Kuller L,LaCroix AZ, Lane D, Langer RD, Lasser N, Lewis CE, Manson J, etal.: Effects of conjugated equine estrogen in postmenopausal womenwith hysterectomy: the Women’s Health Initiative randomized con-trolled trial. JAMA 2004, 291:1701-1712.5. Manson JE, Allison MA, Rossouw JE, Carr JJ, Langer RD, Hsia J,Kuller LH, Cochrane BB, Hunt JR, Ludlam SE, Pettinger MB, Gass M,Margolis KL, Nathan L, Ockene JK, Prentice RL, Robbins J, StefanickML; WHI and WHI-CACS Investigators: Estrogen therapy and coro-nary-artery calcification. N Engl J Med 2007, 356:2591-2602.6. Katayama H, Paczesny S, Prentice R, Aragaki A, Faca VM, Pitteri SJ,Zhang Q, Wnag H, Silva M, Kennedy J, Rossouw J, Jackson R, Hsia J,Chlebowski R, Manson J, Hanash S: Application of serum proteomicsto the Women’s Health Initiative conjugated equine estrogens trialreveals a multitude of effects relevant to clinical findings. GenomeMed 2009, 1:47.http://genomemedicine.com/content/1/6/58 Genome Medicine 2009, Volume 1, Issue 6, Article 58        Veenstra 58.3Genome Medicine 2009, 1:58

Using a Global Proteomic Approach to Identify Proteins Affected by Estrogen Therapy

https://digitalcommons.cedarville.edu/cgi/viewcontent.cgi?article=1283&context=pharmaceutical_sciences_publications

Using a Global Proteomic Approach to Identify Proteins Affected by Estrogen Therapy

Abstract

Similar works

Full text

Available Versions

Digital Commons