Antiapoptotic Herpesvirus Bcl-2 Homologs Escape Caspase-Mediated Conversion to Proapoptotic Proteins

doi:10.1128/JVI.74.11.5024-5031.2000

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Journal of Virology, June 2000, p. 5024-5031, Vol. 74, No. 11
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

Antiapoptotic Herpesvirus Bcl-2 Homologs Escape Caspase-Mediated Conversion to Proapoptotic Proteins

David S. Bellows,¹ B. Nelson Chau,¹ Percy Lee,² Yuri Lazebnik,³ William H. Burns,⁴ and J. Marie Hardwick¹^,²^,^*

Departments of Pharmacology and Molecular Sciences¹ and Molecular Microbiology and Immunology,² Johns Hopkins University Schools of Medicine and Public Health, Baltimore, Maryland 21205; Cold Spring Harbor Laboratory, Cold Spring Harbor, New York, 11724³; and Medical College of Wisconsin, Milwaukee, Wisconsin 53226⁴

Received 14 September 1999/Accepted 2 March 2000

	ABSTRACT

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The antiapoptotic Bcl-2 and Bcl-x_L proteins of mammals are converted into potent proapoptotic factors when they are cleavedby caspases, a family of apoptosis-inducing proteases (E. H.-Y.Cheng, D. G. Kirsch, R. J. Clem, R. Ravi, M. B. Kastan, A. Bedi,K. Ueno, and J. M. Hardwick, Science 278:1966-1968, 1997; R. J.Clem, E. H.-Y. Cheng, C. L. Karp, D. G. Kirsch, K. Ueno, A. Takahashi,M. B. Kastan, D. E. Griffin, W. C. Earnshaw, M. A. Veliuona, andJ. M. Hardwick, Proc. Natl. Acad. Sci. USA 95:554-559, 1998).Gamma herpesviruses also encode homologs of the Bcl-2 family.All tested herpesvirus Bcl-2 homologs possess antiapoptotic activity,including the more distantly related homologs encoded by murinegammaherpesvirus 68 ( $gamma$ HV68) and bovine herpesvirus 4 (BHV4), asdescribed here. To determine if viral Bcl-2 proteins can be convertedinto death factors, similar to their cellular counterparts, fiveherpesvirus Bcl-2 homologs from five different viruses were testedfor their susceptibility to caspases. Only the viral Bcl-2 proteinencoded by $gamma$ HV68 was susceptible to caspase digestion. However,unlike the caspase cleavage products of cellular Bcl-2, Bcl-x_L,and Bid, which are potent inducers of apoptosis, the cleavageproduct of $gamma$ HV68 Bcl-2 lacked proapoptotic activity. KSBcl-2,encoded by the Kaposi's sarcoma-associated herpesvirus, was theonly viral Bcl-2 homolog that was capable of killing cells whenexpressed as an N-terminal truncation. However, because KSBcl-2was not cleavable by caspases, the latent proapoptotic activityof KSBcl-2 apparently cannot be released. The Bcl-2 homologs encodedby herpesvirus saimiri, Epstein-Barr virus, and BHV4 were notcleaved by apoptotic cell extracts and did not possess latentproapoptotic activities. Thus, herpesvirus Bcl-2 homologs escapenegative regulation by retaining their antiapoptotic activitiesand/or failing to be converted into proapoptotic proteins by caspasesduring programmed celldeath.

	INTRODUCTION

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The bcl-2 gene was identified at chromosomal translocation breakpoints in follicular lymphomas and contributes to tumorigenesisby inhibiting programmed cell death rather than by stimulatingcell growth (1, 59). Bcl-2 protein is normally expressedin a wide range of tissues and is required for normal developmentand maintenance of the immune system (61). More than 15 cellularBcl-2-related proteins have been identified in a wide range ofspecies. In addition, Bcl-2 homologs are also found in viral genomes,including oncogenic herpesviruses and the unrelated African swinefever virus (2, 23). Interestingly, all sequenced herpesvirusesof the gamma subfamily, including Epstein-Barr virus (EBV), herpesvirussaimiri (HVS), mouse gammaherpesvirus 68 ( $gamma$ HV68), bovine herpesvirus4 (BHV4) Kaposi's sarcoma-associated herpesvirus (KSHV)/humanherpesvirus 8, equine herpesvirus 2, and ateline herpesvirus 3encode a Bcl-2-like protein, implying a conserved requirementfor viral Bcl-2proteins.

The function of cellular Bcl-2 family members is regulated in part by caspases. We and others have reported that caspase-3cleaves Bcl-2 at Asp-34 and Bcl-x_L at Asp-61 and Asp-76 to produceN-terminally truncated proteins that have lost their antiapoptoticactivities (8, 13, 20, 22, 35). These cleavages arelikely to be physiologically significant, as mutation of the cleavagesites in Bcl-2 and Bcl-x_L enhances their antiapoptotic activities(8, 13). The caspase cleavage products of Bcl-2 and Bcl-x_Lare potently proapoptotic, based on transfection studies expressingprotein fragments that are equivalent to caspase cleavage products(8, 13). Furthermore, apoptosis induced by these fragmentsis blocked by the baculovirus caspase inhibitor P35, suggestingthat these fragments kill cells in a caspase-dependent manner.Thus, the generation of these fragments inside cells may acceleratecell death by amplifying the caspase cascade. In support of thishypothesis, N-terminally truncated Bcl-2 triggers the releaseof cytochrome c from mitochondria, similar to Bax (32, 35).Several groups have found that Bax and Bid are also cleaved duringapoptosis, and their cleavage products are potently proapoptotic(35, 41, 43, 44, 66). Therefore, the cleavage productsof Bcl-2-related proteins may be important facilitators of apoptosisinvivo.

The viral Bcl-2 homologs differ in interesting ways from their cellular counterparts with regard to their effects on cellcycle progression and their abilities to heterodimerize with otherBcl-2 family members (24). Here we report another importantmechanistic difference between viral and cellular Bcl-2 proteins.Herpesvirus Bcl-2 homologs appear to have captured the antiapoptoticfunctions but eliminated the proapoptotic functions of their cellularcounterparts. Thus, these viral proteins may represent constitutivelyactive antiapoptotic versions that escape negative regulationby caspases because they fail to be converted into proapoptoticproteins.

	MATERIALS AND METHODS

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Plasmids and viruses. PCR-amplified full-length or truncated Bcl-2 open reading frames were cloned into pSG5 or a modified pSG5 vector containinga hemagglutinin (HA) epitope tag (pHYC79), and the correct sequencewas confirmed by DNA sequencing. Restriction fragments containingthe HA-tagged or untagged Bcl-2 family members were excised fromthe pSG5 derivatives and inserted at the BstEII site of the Sindbisvirus vector dsTE12Q, and recombinant viruses were generated aspreviously reported (9, 39). Protein expression of the untaggedconstructs was confirmed by in vitro translation with [³⁵S]methionine using T7 quick-coupled TNT (Promega) and resolvedby sodium dodecyl sulfate-polyacrylamide gel electrophoresis (SDS-PAGE)andautoradiography.

Cleavage assays. In vitro cleavage reactions contained 1 µl of ³⁵S-labeled in vitro translation mixture and 1 µl of purified caspase-1 (95 U),caspase-3 (1,600 U), or caspase-8 (260 U), where 1 U generates1 pmol of 7-amino-4-methylcoumarin (AMC) per min by using saturatingsubstrate Ac-YVAD-AMC or Ac-DEVD-AMC (Peptides International)at 25°C. Dithiothreitol was added to a final concentration of10 mM, and caspase reaction buffer (100 mM HEPES [pH 7.5], 10%sucrose, 0.1% CHAPS [3-[(3-cholamidopropyl)-dimethylammonio]-1-propanesulfonate])was added to bring the total reaction volume to 10 µl. After digestionfor 3 h at 37°C, the labeled proteins were analyzed by SDS-PAGEand autoradiography after enhancing with 1 M salicylicacid.

Apoptotic 293 cell extracts were prepared as previously described (18). Cleavage reactions contained 2 µl of ³⁵S-labeled in vitro translation mix and 10 µl of 293 lysate orcaspase reaction buffer. ATP (Boehringer Mannheim) was added toa final concentration of 1 mM, and the reaction mixtures wereincubated at 37°C overnight and analyzed as describedabove.

Virus infection and cell transfection. Low-passage-number (<15) BHK-21 cells (American Type Culture Collection) were infected with 5 PFU of recombinant Sindbis virusvectors per cell in a reduced volume of infection medium (Dulbecco'smodified Eagle's medium supplemented with 1% fetal bovine serum)for 1 h and then returned to 10% serum for 48 h. Infections wereperformed in duplicate, blinded, and at least 500 cells were countedpersample.

BHK-21 or Cos-1 cells were transfected with 0.5 µg of lacZ reporter plasmid pCH110 and various amounts of Bcl-2 plasmid usingLipofectamine (Life Technologies). The total amount of plasmidtransfected was held constant at 2.5 µg by using empty pSG5 vector.Alternatively, Cos-1 cells were transfected with 2 µg of plasmidcontaining procaspase-3 and 0.5 µg of bcl-2 plasmid. At 24 h posttransfection,the cells were fixed with 0.5% glutaraldehyde in phosphate-bufferedsaline and stained with 5-bromo-4-chloro-3-indolyl- $beta$ -D-galactoside(49). Cell viability of blinded samples was determined by countingthe number of blue cells in 10 high-power fields and scoring fornormal versus apoptoticmorphology.

Immunoblot analysis. Cos-1 cells were lysed at 24 h posttransfection in radioimmunoprecipitation assay buffer (150 mM NaCl, 1.0% NP-40, 0.5% deoxycholate,1.0% SDS, 50 mM Tris [pH 8.0]) containing the protease inhibitorsaprotinin, benzamidine, chymostatin, leupeptin, pepstatin A, andphenylmethylsulfonyl fluoride. Protein (50 µg, quantitated bythe bicinchoninic acid assay; Pierce) was separated by SDS-15%PAGE, transferred to nitrocellulose (Schleicher and Schuell),probed with anti-hBcl-2 monoclonal antibody (MAb) (provided byDavid Mason), anti-HA MAb 12CA5 (Berkeley), or anti-caspase-3antibody and detected using SuperSignal(Pierce).

	RESULTS

Top Abstract Introduction Materials and Methods Results Discussion References

Homology domains of viral and cellular Bcl-2 family members. The mammalian Bcl-2 family is defined by the homology domains BH1 to BH4. The most conserved of these are the BH1 and BH2domains, which are important for antiapoptotic activity and dimerization(9, 67). In addition, the BH1-BH2 region spans alpha helices5 and 6, which are implicated in ion channel activity (48).A multiple alignment revealed that the BH1 homology domain isthe most highly conserved domain among gamma herpesvirus Bcl-2homologs (Fig. 1). The BH2 domain is also conserved with the exceptionof $gamma$ HV68, which surprisingly lacks a recognizable BH2 domain (Fig.1). The cell homologs and BHRF1 from Epstein-Barr virus were shownto be anchored to cytoplasmic membranes via their hydrophobicC termini (25, 52). The predicted amino acid sequence forthe other viral genes also contains a stretch of hydrophobic residuesfollowed by one or more positively charged residues at the C terminus.The original BHV4 genome sequence in GenBank apparently containsan error, causing a reading frameshift prior to the hydrophobicC terminus. The sequence of a genomic fragment of BHV4 providedby Vicky Van Santen (Auburn University) contains a 2-nucleotideinsertion at position 615 within the open reading frame (Fig.1). Both $gamma$ HV68 and BHV4 have additional amino acids after thelast charged residue, though the function of this C-terminal extensionis not known. The BH-3 domain is implicated in the cell-killingactivity of the proapoptotic Bcl-2 family members Bax and Bak(11, 64), as well as the Bcl-2 cleavage product (8) andthe more distantly related proteins Bid and Bad (33, 65),but is poorly conserved in the viral homologs. The prodeath activityof the BH3 domain may be linked to its role in dimerization withother Bcl-2 family members. The N-terminal BH4 domain, which isrequired for the antiapoptotic activities of Bcl-2 and Bcl-x_L(27, 30), is poorly conserved even among the cellular homologs.This domain is also poorly conserved in the viral proteins. Similarto Bcl-2 and Bcl-x_L, the Bcl-2 homolog encoded by BHV4 containsa long "loop" domain stretching between BH4 and BH3. However,there is no significant amino acid similarity between any of theviral or cellular loop domains, suggesting that they possess uniquefunctions (Fig. 1). The remaining viral Bcl-2 proteins have muchshorter loop domains, many even shorter than that of Bax.

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FIG. 1. Amino acid alignment of viral and cellular Bcl-2 homologs. Human Bcl-2, human Bcl-x_L, and human Bax are compared with the gammaherpesvirus Bcl-2 homologs ORF16 from KSHV (KSBcl-2), M11 of $gamma$ HV68 ( $gamma$ 68), ORF16 of HVS, BHRF1 of EBV, and BORFB2 of BHV4. Identical (dark shade) and similar (light shade) amino acids occurring in four of the eight entries are marked. Homology domains BH1 to BH4 and the transmembrane domain (TM) are marked with horizontal lines. The caspase recognition sites in Bcl-2 and Bcl-x_L are in bold; arrowheads mark the N termini of truncated mutants. Stars indicate the hydrophobic residues in the BH3 domain of Bak that are important for binding to Bcl-x_L. The GenBank accession number for the corrected sequence data for BORFB2 of BHV4 is AF129421.

$gamma$ HV68 and BHV4 Bcl-2 homologs possess antiapoptotic activity. The viral Bcl-2 homologs from EBV, KSHV, and HVS were shown previously to possess antiapoptotic activity (10, 15, 26,46, 50, 53). Therefore, to determine if the more distantlyrelated Bcl-2 homologs encoded by $gamma$ HV68 and BHV4 also functionas apoptosis inhibitors, they were cloned into the Sindbis virusvector and tested for their ability to inhibit Sindbis virus-inducedapoptosis in BHK cells. Sindbis virus induces all the classicmorphological and biochemical characteristics of apoptosis inmany cell types, including BHK cells, and has proven to be a usefulmodel for studying a variety of cell death regulators, includingviral Bcl-2 proteins (9, 10, 16, 40, 42, 51, 60).Both $gamma$ HV68 and BHV4 Bcl-2 homologs with N-terminal HA tags werecapable of inhibiting apoptosis induced by Sindbis virus almostas efficiently as HA-tagged Bcl-x_L despite lower expression levelsof the BHV4 Bcl-2, as measured by immunoblot analysis with anti-HAantibody (Fig. 2). In contrast, a control protein (chloramphenicolacetyltransferase [CAT]) lacked protective activity when expressedfrom the Sindbis virus vector. Similar to the cellular proteins,deletion of the BH4 domain of $gamma$ HV68 abolished its ability to blockSindbis virus-induced apoptosis (data not shown).

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FIG. 2. BHV4 and $gamma$ HV68 ( $gamma$ 68) Bcl-2 proteins inhibit apoptosis. Apoptotic cell morphology and viability were determined by light microscopy and trypan blue dye exclusion, respectively, at 48 h postinfection of BHK cells with Sindbis virus vectors encoding the indicated Bcl-2 homolog or control CAT. The means and standard errors of the mean (SEM) are shown for three independent experiments. All Bcl-2 homologs have N-terminal HA tags. A corresponding immunoblot analysis with anti-HA antibody is shown.

Viral homologs escape cellular regulatory mechanisms. To determine whether viral Bcl-2 homologs are susceptible to caspase digestion, the viral proteins were translated in vitroand treated with active recombinant purified caspase-1 (whichcleaves Bcl-x_L), caspase-3 (which cleaves Bcl-x_L and Bcl-2), andcaspase-8 (which cleaves Bid). Of the viral proteins, only $gamma$ HV68Bcl-2 was susceptible to partial cleavage by caspase-3 (Fig. 3A),and none of the viral homologs was cleaved by caspase-1 or caspase-8(Fig. 3B) (data not shown). In contrast, Bcl-x_L was cleaved bycaspase-1 to produce a 16-kDa fragment and by caspase-3 to produceboth the 16- and 14-kDa fragments observed previously in vitroand in apoptotic cells (13, 20).

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FIG. 3. Except for $gamma$ HV68 ( $gamma$ 68) Bcl-2, viral Bcl-2 homologs are not cleaved by caspases. The indicated ³⁵S-labeled, in vitro-translated proteins were digested with the indicated recombinant caspases or incubated with caspase buffer only (lane $---$ ). Proteins were analyzed by SDS-PAGE and autoradiography. Caspase activity was determined by using peptide substrates as described in Materials and Methods. Minor bands that are present in both digested and undigested lanes are presumably premature terminations, internal initiations, or nonspecific degradation products. For example, the ~26-kDa fragment of Bcl-x_L is due to initiation at an internal Met at position 45 (13). Molecular size markers are indicated (in kilodaltons). Brackets indicate the approximate positions of viral proteins lacking the N-terminal BH4 domain.

To further explore the possibility that viral Bcl-2 homologs could be cleaved by caspases or other proteases during apoptosis,in vitro-translated proteins were treated with apoptotic extractsprepared from 293 cells, which contain a number of activated caspases(18). Again only Bcl-x_L and $gamma$ HV68 Bcl-2 were cleaved (Fig. 4Aand B). By analogy with Bcl-2 and Bcl-x_L, the $gamma$ HV68 homolog isexpected to be cleaved in the loop region between BH4 and BH3.Immunoblot analysis verified that the $gamma$ HV68 protease site is locatedin the N terminus, because the cleavage product is not detectedwith an antibody to the N-terminal HA tag (data not shown). Caspasescleave exclusively after Asp residues, and there are three Aspresidues present in the loop region of $gamma$ HV68 Bcl-2 (residues 28,31, and 37). The consensus cleavage site for caspase-3 is DXXD(58), consistent with the $gamma$ HV68 Bcl-2 sequence DCVD³¹ (bold in Fig. 1). Furthermore, the cleavage product of $gamma$ HV68Bcl-2 migrates only slightly faster than that of a deletion mutantlacking amino acids 2 to 28 ( $Delta$ N28), consistent with cleavage atAsp-31, Asp-37, or both (Fig. 4, compare last two lanes). Exceptfor KSBcl-2, encoded by KSHV, the viral Bcl-2 proteins containat least one Asp residue in this region, though none is a consensuscaspase-3 site. Other sequences as well as structural featuresare required to constitute a caspase cleavage site because caspasesare known to cleave only at specific Asp residues. Therefore,it appears that caspases cleave and inactivate only one of theherpesvirus Bcl-2 homologs tested. However, it is not known ifcaspase cleavage of $gamma$ HV68 Bcl-2 occurs during virus infectionof mice.

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FIG. 4. Except for $gamma$ HV68 ( $gamma$ 68) Bcl-2, viral Bcl-2 proteins are resistant to cleavage by apoptotic cell extracts. In vitro-translated, ³⁵S-labeled proteins were digested with apoptotic 293 cell extracts (18). Proteins were analyzed by SDS-PAGE and autoradiography. Treated and untreated samples were run on the same gel with the same exposure, though the lanes were rearranged for display. Longer gels confirmed the absence of detectable small cleavage products (data not shown). For an explanation of minor bands in both digested and undigested samples, see the legend to Fig. 3. Molecular size markers are indicated (in kilodaltons). wt, wild type.

To determine whether viral Bcl-2 proteins harbor latent proapoptotic activity, C-terminal fragments of the viral proteinswere expressed in transfected cells. Constructs were generatedto mimic potential caspase cleavage fragments, such that all truncatedproteins lacked the BH4 homology domain and retained the BH3 domain.The arrowheads in Fig. 1 mark the new N termini (plus an initiationMet). The exact positions of the newly generated N termini maynot be critical, as the position of the caspase cleavage siteis not conserved between Bcl-2 and Bcl-x_L. That is, Bcl-2 is cleavedon the N-terminal side of the ~50-amino-acid loop domain, whileBcl-x_L is cleaved on the C-terminal side of the loop (bold inFig. 1). Furthermore, the 16-kDa Bcl-x_L, 14-kDa Bcl-x_L, and 23-kDaBcl-2 fragments all possess equivalent proapoptotic activitiesin cultured cells (8, 20) (data not shown). Transfectionof the N-terminally truncated viral Bcl-2 constructs had no effecton cell viability except for $Delta$ N20 KSBcl-2, which killed cellsin a dose-dependent manner, similar to $Delta$ N61 Bcl-x_L (16-kDa fragment)(Fig. 5). Similar results were obtained in Cos-1 cells (data notshown). However, because the KSBcl-2 protein has no potentialcaspase cleavage sites between BH4 and BH3 and was not cleavedby recombinant caspases or apoptotic cell extracts, its proapoptoticfunction appears to remain latent. The caspase cleavage productof $gamma$ HV68 Bcl-2, the only cleavable viral homolog, was not capableof killing BHK cells (Fig. 5). Similar results were obtained inCos-1 cells (data not shown). Because of the lack of appropriateantibodies and because N- and C-terminal tags impair the prodeathactivities of truncated Bcl-x_L and KSBcl-2, all fragments wereexpressed without tags. Therefore, all plasmid inserts were completelysequenced, and protein expression was confirmed by in vitro translationof the same plasmids used for transfection (Fig. 4 and data notshown).

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FIG. 5. Except for $Delta$ N20 KSBcl-2, N-terminally truncated viral Bcl-2 proteins lack proapoptotic activity. Plasmids encoding wild-type Bcl-2 family members or N-terminal truncations lacking the indicated number of amino acids were transfected into BHK cells at the indicated DNA concentrations. Cell viability was determined at 24 h posttransfection by scoring the percentage of live/nonapoptotic versus total transfected cells (counting >250 lacZ-positive cells per sample). The data presented are the means and SEM for three to six independent experiments.

These findings suggest that viral Bcl-2 homologs escape cellular regulatory mechanisms by retaining their antiapoptotic activitiesand/or by failing to be converted into proapoptotic proteins whencaspases are activated during apoptosis. To compare KSBcl-2 witha cellular homolog in the presence of activated caspases, cellviability was monitored in Cos-1 cells that had been transfectedwith procaspase-3 and a Bcl-2 homolog (Fig. 6). Caspase-3 wasselected for this experiment because it is an abundant downstreamcaspase and the only caspase that cleaves viral and cellular Bcl-2proteins (35). Overexpression of procaspase-3 alone had no effecton cell viability. However, overexpression of Bcl-2 alone exhibitedsome intrinsic proapoptotic activity, a phenomenon previouslyobserved in many laboratories, including ours (8). When procaspase-3was cotransfected with human Bcl-2, cell viability was furtherreduced concomitant with cleavage of Bcl-2 to its 23-kDa signaturefragment. The Bcl-2 cleavage product was shown previously to activatecaspases by inducing release of cytochrome c from mitochondriain a feed-forward pathway to accelerate cell death (35). Consistentwith this finding, cotransfection of Bcl-2 and procaspase-3 resultedin processing of procaspase-3 to its active form (Fig. 6). Thecaspase-3-mediated enhancement of cell death was abolished bymutation of the caspase-3 cleavage site in Bcl-2 (D34A). The faintBcl-2 cleavage product observed with the D34A mutant in the presenceof caspase-3 is probably due to inefficient cleavage at Asp-31(the P4 position in the DAGD³⁴ site). Taken together, these data indicate that the cell killingfunction of Bcl-2 is enhanced when the proapoptotic fragment ofBcl-2 is released by caspase cleavage. The observation that Bcl-2induced cell death (without cotransfected caspase-3) suggeststhat the proapoptotic function of full-length Bcl-2 may be unleashedby mechanisms other than caspase cleavage. In contrast to humanBcl-2, KSBcl-2 lacked intrinsic proapoptotic activity and failedto enhance cell death relative to the control vector when cotransfectedwith procaspase-3 (Fig. 6). In addition, KSBcl-2 had almost noability to induce the processing of procaspase-3 to its activeform. Thus, KSBcl-2 was not converted to a proapoptotic form bycaspase-3 or other cell factors.

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FIG. 6. Antiapoptotic activity of KSBcl-2 is resistant to inactivation by caspase-3. Cell viability of Cos-1 cells transfected with the indicated plasmids was determined as described in the legend to Fig. 5. The data are the means and SEM. The effect of cotransfected procaspase-3 was statistically significant only for wild-type Bcl-2 using a Wilcoxon signed-rank test for paired analysis of seven independent experiments (indicated at the top). Representative immunoblots of transfected cell lysates with the indicated antibodies are shown below. Pro, unprocessed form of procaspase-3; Act, active cleavage product of caspase-3.

	DISCUSSION

Top Abstract Introduction Materials and Methods Results Discussion References

Herpesvirus genomes contain large blocks of conserved genes required for housekeeping functions. These blocks are separatedby genes that are unique to herpesvirus subfamilies or uniqueto a particular virus. Unlike other herpesviruses, the gammaherpesvirussubfamily encodes a number of proteins with obvious homology tocellular factors, such as cyclin D, OX2, interleukin-8 receptor,interleukin-6, chemokines, chemokine receptors, interferon regulatoryfactors, FLIP proteins, Bcl-2, and others (21). These factorswere presumably acquired as adaptations to a particular host environmentand are candidate perpetrators of the distinct diseases and cancersassociated with these viruses. Some of these viral homologs haveexpanded functions or escape regulatory mechanisms to which theircellular counterparts are subject. KSHV encodes a G-protein-coupledreceptor (ORF74) that stimulates cell proliferation and angiogenesisby a constitutive, agonist-independent mechanism (3, 5).The viral chemokine encoded by KSHV, vMIP-II, binds to a broaderrange of receptors with higher affinity, functions as an antagonistof chemotaxis, and is a potent angiogenic factor, unlike cellularMIP-1 $alpha$ and RANTES (7, 36). Our data suggest that like thesefactors, the gammaherpesvirus Bcl-2 homologs may be constitutivelyactive. In this way, viral Bcl-2 proteins are unlike several cellularBcl-2 family members that become potent killer proteins followingproteolytic cleavage. Consistent with this model, HVS Bcl-2 wasshown to protect Jurkat cells from Fas-induced apoptosis, in contrastto human Bcl-2, which is cleaved by caspases in Jurkat cells followingFas ligation (8, 15). While our paper was in review, Wanget al. reported that $gamma$ HV68 Bcl-2 inhibits Fas- and tumor necrosisfactor-induced apoptosis in HeLa cells (63). Therefore, theSindbis virus-induced apoptosis utilized in our studies also reflectsthe results obtained with other cell deathstimuli.

Viral Bcl-2 proteins differ in other ways from their cellular homologs. In contrast to Bcl-2, which suppresses cell cycleprogression (28), BHRF1 was reported to stimulate cell cycleprogression in some situations (14, 29). However, anothergroup reported that BHRF1 interferes with Ras-induced proliferation,which can be relieved by amino acid substitutions in the BH3 domainof BHRF1 (56). These disparate results could potentially beexplained by cell type-specific factors that modulate BHRF1 function(19).

Like human Bcl-2, herpesvirus Bcl-2 homologs can cooperate with adenovirus E1A and c-Myc to facilitate cell transformation(17, 56), raising the possibility that viral Bcl-2 proteinsmay contribute directly to the tumorigenic potential of severalof these viruses. This is consistent with the finding that the $gamma$ HV68 Bcl-2 homolog appears to be expressed during latency ininfected mice (62). In addition, viral Bcl-2 homologs may serveto prevent premature cell death during virus replication, fittingwith the observation that several of the viral Bcl-2 homologsare synthesized during the lytic phase of the virus life cycle(4, 10). Although an EBV mutant lacking its Bcl-2 homolog(BHRF1) has no detectable phenotype in cell culture (38, 45),natural isolates of EBV retain a functional BHRF1, further suggestingits importance to the biology of the virus (34). However, byanalogy with other large DNA viruses, antiapoptotic functionsmay be redundantly encoded (23). In fact, a second Bcl-2 homologencoded by EBV was recently reported (46). Furthermore, theKSHV, equine herpesvirus 2, BHV4, HVS, and ateline herpesvirus3 viruses all encode viral FLIP proteins that are implicated inblocking caspase recruitment to cell death receptors (6, 57).

The BH3 domain is required and sufficient for the proapoptotic activity of Bax and Bak in some assays (8, 11). Giventhat the viral Bcl-2 proteins have lost their latent proapoptoticactivities (except for KSBcl-2), it is not surprising that theBH3 domain is less well conserved in the viral proteins. Basedon the nuclear magnetic resonance structure of a peptide of Bakbound to Bcl-x_L, the BH3 domain of Bak forms an alpha-helix thatinserts into a hydrophobic cleft on Bcl-x_L, probably inactivatingits antiapoptotic activity (54). A comparison of the structuresof cleaved and uncleaved Bid suggests that cleavage of Bid bycaspase-8 exposes the Bid BH3 domain and may contribute to reorientationof the Bid BH3 domain, making it more available for binding partners(12, 47). Of the four hydrophobic amino acids in the Bak/BidBH3 domain that insert into the hydrophobic groove on Bcl-x_L,only three of these are conserved in the viral homologs (the positionsof these hydrophobic amino acids are marked with stars in Fig.1). However, in comparing their BH3 domains, it is not apparentwhy N-terminally truncated KSBcl-2 possesses proapoptotic activitywhile the other viral proteins lack this activity. Perhaps a cleavage-dependentconformational change that exposes the binding face of the BH3domain of Bcl-2 and Bcl-x_L does not occur in the herpesvirushomologs.

The role of heterodimerization between proapoptotic and antiapoptotic Bcl-2 family members in blocking cell death is not fullyunderstood. Although Bcl-2 and Bcl-x_L can prevent cell death bymechanisms other than sequestering Bax and Bak, heterodimerizationmay serve to titrate the intracellular concentrations of thesepartners (9, 37). However, no consistent picture has emergedwith regard to heterodimerization of viral Bcl-2 proteins. HVSBcl-2 appears to be capable of binding and perhaps suppressingthe activity of Bax (10, 50, 56), while other viral homologsfail to heterodimerize with Bax (e.g., KSBcl-2 and BHRF1) andpotentially escape inactivation by Bax. KSBcl-2 was recently demonstratedto bind a new member of the Bcl-2 family, Diva/Boo, though thereis controversy about whether Diva/Boo is an antiapoptotic or proapoptoticprotein (31, 55). Like Bcl-2, Bcl-x_L, and perhaps Diva/Boo,Bax can also flip its function and become an antiapoptotic factor(41). Thus, while both pro- and antiapoptotic cellular Bcl-2family proteins can reverse their functions, viral Bcl-2 homologsappear to be locked into the antiapoptoticmode.

The inability of herpesvirus Bcl-2 proteins to be cleaved by caspases and their lack of proapoptotic activity strongly indicatethat these viral factors have eliminated key features of the cellularhomologs from which they were likely derived. If low levels ofcaspases become activated in healthy cells, the generation ofproapoptotic fragments from target substrates such as Bcl-2 familyproteins may be necessary to amplify the apoptotic pathway andfacilitate cell death. Indeed, the cleavage fragment of Bcl-2and Bid can induce the release of cytochrome c from mitochondria(35, 43). Cytochrome c serves as an essential cofactor forApaf-1 to activate procaspase-9, which in turn amplifies the caspasecascade (68). Overexpression of viral Bcl-2 proteins that failto facilitate cell death could potentially serve to tip the balancein favor of cellsurvival.

	ACKNOWLEDGMENTS

We thank Vicky van Santen for BHV4 DNA, John Nicholas for HVS DNA, and Nancy Thornberry for purifiedcaspases.

This work was supported by research grant RO1 CA73581 from the National Institutes of Health (J.M.H.).

	FOOTNOTES

^* Corresponding author. Mailing address: Dept. of Molecular Microbiology and Immunology, Johns Hopkins, E5132 SPH, 615 NorthWolfe St., Baltimore, MD 21205. Phone: (410) 955-2716. Fax: (410)955-0105. E-mail: hardwick{at}jhu.edu.

REFERENCES

Top
Abstract
Introduction
Materials and Methods
Results
Discussion
References

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