Your search keyword '"Riggs DL"' showing total 38 results

1. Transcriptional Heterogeneity Overcomes Super-Enhancer Disrupting Drug Combinations in Multiple Myeloma.

Author

Welsh SJ, Barwick BG, Meermeier EW, Riggs DL, Shi CX, Zhu YX, Sharik ME, Du MT, Abrego Rocha LD, Garbitt VM, Stein CK, Petit JL, Meurice N, Tafoya Alvarado Y, Fonseca R, Todd KT, Brown S, Hammond ZJ, Cuc NH, Wittenberg C, Herzog C, Roschke AV, Demchenko YN, Chen WD, Li P, Liao W, Leonard WJ, Lonial S, Bahlis NJ, Neri P, Boise LH, Chesi M, and Bergsagel PL

Subjects

Humans, Lenalidomide pharmacology, Lenalidomide therapeutic use, Transcription Factor AP-1 therapeutic use, Drug Combinations, Immunomodulating Agents, Multiple Myeloma drug therapy, Multiple Myeloma genetics

Abstract

Multiple myeloma (MM) is a malignancy that is often driven by MYC and that is sustained by IRF4, which are upregulated by super-enhancers. IKZF1 and IKZF3 bind to super-enhancers and can be degraded using immunomodulatory imide drugs (IMiD). Successful IMiD responses downregulate MYC and IRF4; however, this fails in IMiD-resistant cells. MYC and IRF4 downregulation can also be achieved in IMiD-resistant tumors using inhibitors of BET and EP300 transcriptional coactivator proteins; however, in vivo these drugs have a narrow therapeutic window. By combining IMiDs with EP300 inhibition, we demonstrate greater downregulation of MYC and IRF4, synergistic killing of myeloma in vitro and in vivo, and an increased therapeutic window. Interestingly, this potent combination failed where MYC and IRF4 expression was maintained by high levels of the AP-1 factor BATF. Our results identify an effective drug combination and a previously unrecognized mechanism of IMiD resistance., Significance: These results highlight the dependence of MM on IKZF1-bound super-enhancers, which can be effectively targeted by a potent therapeutic combination pairing IMiD-mediated degradation of IKZF1 and IKZF3 with EP300 inhibition. They also identify AP-1 factors as an unrecognized mechanism of IMiD resistance in MM. See related article by Neri, Barwick, et al., p. 56. See related commentary by Yun and Cleveland, p. 5. This article is featured in Selected Articles from This Issue, p. 4., (©2023 The Authors; Published by the American Association for Cancer Research.)

Published

2024

2. ETV4-Dependent Transcriptional Plasticity Maintains MYC Expression and Results in IMiD Resistance in Multiple Myeloma.

Author

Neri P, Barwick BG, Jung D, Patton JC, Maity R, Tagoug I, Stein CK, Tilmont R, Leblay N, Ahn S, Lee H, Welsh SJ, Riggs DL, Stong N, Flynt E, Thakurta A, Keats JJ, Lonial S, Bergsagel PL, Boise LH, and Bahlis NJ

Subjects

Humans, Bromodomain Containing Proteins, Cell Cycle Proteins, Immunomodulating Agents, Neoplasm Recurrence, Local, Nuclear Proteins, Proto-Oncogene Proteins c-ets genetics, Transcription Factors genetics, Ubiquitin-Protein Ligases physiology, Ubiquitin-Protein Ligases therapeutic use, Multiple Myeloma drug therapy, Multiple Myeloma genetics

Abstract

Immunomodulatory drugs (IMiD) are a backbone therapy for multiple myeloma (MM). Despite their efficacy, most patients develop resistance, and the mechanisms are not fully defined. Here, we show that IMiD responses are directed by IMiD-dependent degradation of IKZF1 and IKZF3 that bind to enhancers necessary to sustain the expression of MYC and other myeloma oncogenes. IMiD treatment universally depleted chromatin-bound IKZF1, but eviction of P300 and BRD4 coactivators only occurred in IMiD-sensitive cells. IKZF1-bound enhancers overlapped other transcription factor binding motifs, including ETV4. Chromatin immunoprecipitation sequencing showed that ETV4 bound to the same enhancers as IKZF1, and ETV4 CRISPR/Cas9-mediated ablation resulted in sensitization of IMiD-resistant MM. ETV4 expression is associated with IMiD resistance in cell lines, poor prognosis in patients, and is upregulated at relapse. These data indicate that ETV4 alleviates IKZF1 and IKZF3 dependency in MM by maintaining oncogenic enhancer activity and identify transcriptional plasticity as a previously unrecognized mechanism of IMiD resistance., Significance: We show that IKZF1-bound enhancers are critical for IMiD efficacy and that the factor ETV4 can bind the same enhancers and substitute for IKZF1 and mediate IMiD resistance by maintaining MYC and other oncogenes. These data implicate transcription factor redundancy as a previously unrecognized mode of IMiD resistance in MM. See related article by Welsh, Barwick, et al., p. 34. See related commentary by Yun and Cleveland, p. 5. This article is featured in Selected Articles from This Issue, p. 4., (©2023 The Authors; Published by the American Association for Cancer Research.)

Published

2024

3. Statistical Framework for Identifying Differences in Similar Mass Spectra: Expanding Possibilities for Isomer Identification.

Author

Wu HT, Riggs DL, Lyon YA, and Julian RR

Subjects

Chromatography, Liquid methods, Isomerism, Tandem Mass Spectrometry methods, Peptides

Abstract

Isomeric molecules are important analytes in many biological and chemical arenas, yet their similarity poses challenges for many analytical methods, including mass spectrometry (MS). Tandem-MS provides significantly more information about isomers than intact mass analysis, but highly similar fragmentation patterns are common and include cases where no unique m / z peaks are generated between isomeric pairs. However, even in such situations, differences in peak intensity can exist and potentially contain additional information. Herein, we present a framework for comparing mass spectra that differ only in terms of peak intensity and include calculation of a statistical probability that the spectra derive from different analytes. This framework allows for confident identification of peptide isomers by collision-induced dissociation, higher-energy collisional dissociation, electron-transfer dissociation, and radical-directed dissociation. The method successfully identified many types of isomers including various d/l amino acid substitutions, Leu/Ile, and Asp/IsoAsp. The method can accommodate a wide range of changes in instrumental settings including source voltages, isolation widths, and resolution without influencing the analysis. It is shown that quantification of the composition of isomeric mixtures can be enabled with calibration curves, which were found to be highly linear and reproducible. The analysis can be implemented with data collected by either direct infusion or liquid-chromatography MS. Although this framework is presented in the context of isomer characterization, it should also prove useful in many other contexts where similar mass spectra are generated.

Published

2023

4. Tumor burden limits bispecific antibody efficacy through T cell exhaustion averted by concurrent cytotoxic therapy.

Author

Meermeier EW, Welsh SJ, Sharik ME, Du MT, Garbitt VM, Riggs DL, Shi CX, Stein CK, Bergsagel M, Chau B, Wheeler ML, Bezman N, Wang F, Strop P, Bergsagel PL, and Chesi M

Subjects

Animals, Humans, Immunotherapy, Mice, T-Lymphocytes, Tumor Burden, Antibodies, Bispecific pharmacology, Multiple Myeloma drug therapy

Abstract

BCMA-CD3-targeting bispecific antibodies (BsAb) are a recently developed immunotherapy class which shows potent tumor killing activity in multiple myeloma (MM). Here, we investigated a murine BCMA-CD3-targeting BsAb in the immunocompetent Vk*MYC and its IMiD-sensitive derivative Vk*MYC hCRBN models of MM. The BCMA-CD3 BsAb was safe and efficacious in a subset of mice, but failed in those with high-tumor burden, consistent with clinical reports of BsAb in leukemia. The combination of BCMA-CD3 BsAb with pomalidomide expanded lytic T cells and improved activity even in IMiD resistant high-tumor burden cases. Yet, survival was only marginally extended due to acute toxicity and T cell exhaustion, which impaired T cell persistence. In contrast, the combination with cyclophosphamide was safe and allowed for a tempered pro-inflammatory response associated with long-lasting complete remission. Concurrent cytotoxic therapy with BsAb actually improved T cell persistence and function, offering a promising approach to patients with a large tumor burden.

Published

2021

5. Monosomic loss of MIR15A/MIR16-1 is a driver of multiple myeloma proliferation and disease progression.

Author

Chesi M, Stein CK, Garbitt VM, Sharik ME, Asmann YW, Bergsagel M, Riggs DL, Welsh SJ, Meermeier EW, Kumar SK, Braggio E, and Bergsagel PL

Subjects

Animals, Cell Proliferation genetics, Disease Progression, Humans, Mice, Leukemia, Lymphocytic, Chronic, B-Cell genetics, MicroRNAs genetics, Monoclonal Gammopathy of Undetermined Significance genetics, Multiple Myeloma genetics, Multiple Myeloma pathology

Abstract

The most common genetic abnormality in multiple myeloma (MM) is the deletion of chromosome 13, seen in almost half of newly diagnosed patients. Unlike chronic lymphocytic leukemia, where a recurrent minimally deleted region including MIR15A/MIR16-1 has been mapped, the deletions in MM predominantly involve the entire chromosome and no specific driver gene has been identified. Additional candidate loci include RB1 and DIS3 , but while biallelic deletion of RB1 is associated with disease progression, DIS3 is a common essential gene and complete inactivation is not observed. The Vk*MYC transgenic mouse model of MM spontaneously acquires del(14), syntenic to human chromosome 13, and Rb1 complete inactivation, but not Dis3 mutations. Taking advantage of this model, we explored the role in MM initiation and progression of two candidate loci on chromosome 13: RB1 and MIR15A/MIR16-1 . Monoallelic deletion of Mir15a/Mir16-1 but not Rb1 was sufficient to accelerate the development of monoclonal gammopathy in wildtype mice, and the progression of MM in Vk*MYC mice, resulting in increased expression of Mir15a/Mir16-1 target genes and plasma cell proliferation, which was similarly observed in patients with MM., Competing Interests: The authors declare no potential conflicts of interest

Published

2020

6. MYC dysregulation in the progression of multiple myeloma.

Author

Misund K, Keane N, Stein CK, Asmann YW, Day G, Welsh S, Van Wier SA, Riggs DL, Ahmann G, Chesi M, Viswanatha DS, Kumar SK, Dispenzieri A, Gonzalez-Calle V, Kyle RA, O'Dwyer M, Rajkumar SV, Kortüm KM, Keats JJ, Fonseca R, Stewart AK, Kuehl WM, Braggio E, and Bergsagel PL

Subjects

Disease Progression, Humans, Multiple Myeloma genetics, Mutation, Multiple Myeloma pathology, Proto-Oncogene Proteins c-myc genetics

Published

2020

7. Mate pair sequencing outperforms fluorescence in situ hybridization in the genomic characterization of multiple myeloma.

Author

Smadbeck J, Peterson JF, Pearce KE, Pitel BA, Figueroa AL, Timm M, Jevremovic D, Shi M, Stewart AK, Braggio E, Riggs DL, Bergsagel PL, Vasmatzis G, Kearney HM, Hoppman NL, Ketterling RP, Kumar S, Rajkumar SV, Greipp PT, and Baughn LB

Subjects

Adult, Aged, Aged, 80 and over, Bone Marrow pathology, Bone Marrow Cells metabolism, Bone Marrow Cells pathology, Chromosome Aberrations, Female, Gene Rearrangement, Genes, myc, Humans, Male, Middle Aged, Reproducibility of Results, Genetic Variation, Genomics methods, Genomics standards, In Situ Hybridization, Fluorescence methods, In Situ Hybridization, Fluorescence standards, Multiple Myeloma diagnosis, Multiple Myeloma genetics

Abstract

Fluorescence in situ hybridization (FISH) is currently the gold-standard assay to detect recurrent genomic abnormalities of prognostic significance in multiple myeloma (MM). Since most translocations in MM involve a position effect with heterogeneous breakpoints, we hypothesize that FISH has the potential to miss translocations involving these regions. We evaluated 70 bone marrow samples from patients with plasma cell dyscrasia by FISH and whole-genome mate-pair sequencing (MPseq). Thirty cases (42.9%) displayed at least one instance of discordance between FISH and MPseq for each primary and secondary abnormality evaluated. Nine cases had abnormalities detected by FISH that went undetected by MPseq including 6 tetraploid clones and three cases with missed copy number abnormalities. In contrast, 19 cases had abnormalities detected by MPseq that went undetected by FISH. Seventeen were MYC rearrangements and two were 17p deletions. MPseq identified 36 MYC abnormalities and 17 (50.0% of MYC abnormal group with FISH results) displayed a false negative FISH result. MPseq identified 10 cases (14.3%) with IgL rearrangements, a recent marker of poor outcome, and 10% with abnormalities in genes associated with lenalidomide response or resistance. In summary, MPseq was superior in the characterization of rearrangement complexity and identification of secondary abnormalities demonstrating increased clinical value compared to FISH.

Published

2019

8. Analysis of Glutamine Deamidation: Products, Pathways, and Kinetics.

Author

Riggs DL, Silzel JW, Lyon YA, Kang AS, and Julian RR

Subjects

Chromatography, Liquid, Crystallins chemistry, Crystallins metabolism, Glutamine metabolism, Humans, Hydrolysis, Iodobenzoates chemistry, Kinetics, Lens, Crystalline chemistry, Mass Spectrometry, Time Factors, Crystallins analysis, Glutamine analogs & derivatives, Glutamine analysis

Abstract

Spontaneous chemical modifications play an important role in human disease and aging at the molecular level. Deamidation and isomerization are known to be among the most prevalent chemical modifications in long-lived human proteins and are implicated in a growing list of human pathologies, but the relatively minor chemical change associated with these processes has presented a long standing analytical challenge. Although the adoption of high-resolution mass spectrometry has greatly aided the identification of deamidation sites in proteomic studies, isomerization (and the isomeric products of deamidation) remain exceptionally challenging to characterize. Herein, we present a liquid chromatography/mass spectrometry-based approach for rapidly characterizing the isomeric products of Gln deamidation using diagnostic fragments that are abundantly produced and capable of unambiguously identifying both Glu and isoGlu. Importantly, the informative fragment ions are produced through orthogonal fragmentation pathways, thereby enabling the simultaneous detection of both isomeric forms while retaining compatibility with shotgun proteomics. Furthermore, the diagnostic fragments associated with isoGlu pinpoint the location of the modified residue. The utility of this technique is demonstrated by characterizing the isomeric products generated during in vitro aging of a series of glutamine-containing peptides. Sequence-dependent product profiles are obtained, and the abundance of deamidation-linked racemization is examined. Finally, comparisons are made between Gln deamidation, which is relatively poorly understood, and asparagine deamidation, which has been more thoroughly studied.

Published

2019

9. Spontaneous Isomerization of Long-Lived Proteins Provides a Molecular Mechanism for the Lysosomal Failure Observed in Alzheimer's Disease.

Author

Lambeth TR, Riggs DL, Talbert LE, Tang J, Coburn E, Kang AS, Noll J, Augello C, Ford BD, and Julian RR

Abstract

Proteinaceous aggregation is a well-known observable in Alzheimer's disease (AD), but failure and storage of lysosomal bodies within neurons is equally ubiquitous and actually precedes bulk accumulation of extracellular amyloid plaque. In fact, AD shares many similarities with certain lysosomal storage disorders though establishing a biochemical connection has proven difficult. Herein, we demonstrate that isomerization and epimerization, which are spontaneous chemical modifications that occur in long-lived proteins, prevent digestion by the proteases in the lysosome (namely, the cathepsins). For example, isomerization of aspartic acid into l-isoAsp prevents digestion of the N-terminal portion of Aβ by cathepsin L, one of the most aggressive lysosomal proteases. Similar results were obtained after examination of various target peptides with a full series of cathepsins, including endo-, amino-, and carboxy-peptidases. In all cases peptide fragments too long for transporter recognition or release from the lysosome persisted after treatment, providing a mechanism for eventual lysosomal storage and bridging the gap between AD and lysosomal storage disorders. Additional experiments with microglial cells confirmed that isomerization disrupts proteolysis in active lysosomes. These results are easily rationalized in terms of protease active sites, which are engineered to precisely orient the peptide backbone and cannot accommodate the backbone shift caused by isoaspartic acid or side chain dislocation resulting from epimerization. Although Aβ is known to be isomerized and epimerized in plaques present in AD brains, we further establish that the rates of modification for aspartic acid in positions 1 and 7 are fast and could accrue prior to plaque formation. Spontaneous chemistry can therefore provide modified substrates capable of inducing gradual lysosomal failure, which may play an important role in the cascade of events leading to the disrupted proteostasis, amyloid formation, and tauopathies associated with AD., Competing Interests: The authors declare no competing financial interest.

Published

2019

10. Structural and functional consequences of age-related isomerization in α-crystallins.

Author

Lyon YA, Collier MP, Riggs DL, Degiacomi MT, Benesch JLP, and Julian RR

Subjects

Humans, Phosphorylation, Protein Domains, alpha-Crystallin A Chain metabolism, alpha-Crystallin B Chain metabolism, Aging, Protein Aggregates, Protein Multimerization, alpha-Crystallin A Chain chemistry, alpha-Crystallin B Chain chemistry

Abstract

Long-lived proteins are subject to spontaneous degradation and may accumulate a range of modifications over time, including subtle alterations such as side-chain isomerization. Recently, tandem MS has enabled identification and characterization of such peptide isomers, including those differing only in chirality. However, the structural and functional consequences of these perturbations remain largely unexplored. Here, we examined the impact of isomerization of aspartic acid or epimerization of serine at four sites mapping to crucial oligomeric interfaces in human αA- and αB-crystallin, the most abundant chaperone proteins in the eye lens. To characterize the effect of isomerization on quaternary assembly, we utilized synthetic peptide mimics, enzyme assays, molecular dynamics calculations, and native MS experiments. The oligomerization of recombinant forms of αA- and αB-crystallin that mimic isomerized residues deviated from native behavior in all cases. Isomerization also perturbs recognition of peptide substrates, either enhancing or inhibiting kinase activity. Specifically, epimerization of serine (αASer-162) dramatically weakened inter-subunit binding. Furthermore, phosphorylation of αBSer-59, known to play an important regulatory role in oligomerization, was severely inhibited by serine epimerization and altered by isomerization of nearby αBAsp-62. Similarly, isomerization of αBAsp-109 disrupted a vital salt bridge with αBArg-120, a contact that when broken has previously been shown to yield aberrant oligomerization and aggregation in several disease-associated variants. Our results illustrate how isomerization of amino acid residues, which may seem to be only a minor structural perturbation, can disrupt native structural interactions with profound consequences for protein assembly and activity., (© 2019 Lyon et al.)

Published

2019

11. Identification of lenalidomide resistance pathways in myeloma and targeted resensitization using cereblon replacement, inhibition of STAT3 or targeting of IRF4.

Author

Zhu YX, Shi CX, Bruins LA, Wang X, Riggs DL, Porter B, Ahmann JM, de Campos CB, Braggio E, Bergsagel PL, and Stewart AK

Subjects

Biomarkers, Tumor, Cell Line, Tumor, Comparative Genomic Hybridization, Cytokines, Gene Expression, Humans, Immunomodulation drug effects, Lenalidomide therapeutic use, Models, Biological, Multiple Myeloma drug therapy, Multiple Myeloma genetics, Multiple Myeloma immunology, Protein Binding, Ubiquitin-Protein Ligases, Adaptor Proteins, Signal Transducing metabolism, Drug Resistance, Neoplasm genetics, Interferon Regulatory Factors antagonists & inhibitors, Lenalidomide pharmacology, Multiple Myeloma metabolism, STAT3 Transcription Factor antagonists & inhibitors, Signal Transduction drug effects

Abstract

To understand immunomodulatory drug (IMiD) resistance in multiple myeloma (MM), we created isogenic human multiple myeloma cell lines (HMCLs) sensitive and resistant to lenalidomide, respectively. Four HMCLs were demonstrated to be resistant to all IMiDs including lenalidomide, pomalidomide, and CC-220, but not to Bortezomib. In three HMLCs (MM.1.SLenRes, KMS11LenRes and OPM2LenRes), CRBN abnormalities were found, including chromosomal deletion, point mutation, and low CRBN expression. The remaining HMCL, XG1LenRes, showed no changes in CRBN but exhibited CD147 upregulation and impaired IRF4 downregulation after lenalidomide treatment. Depletion of CD147 in XG1LenRes and three additional HMCLs had no significant impact on MM viability and lenalidomide response. Further analysis of XG1LenRes demonstrated increased IL6 expression and constitutive STAT3 activation. Inhibition of STAT3 with a selective compound (PB-1-102) re-sensitized XG1LenRes to lenalidomide. Since XG1LenRes harbors a truncated IRF4 that is not downregulated by lenalidomide, we targeted IRF4/MYC axis with a selective inhibitor of the bromodomain of CBP/EP300 (SGC-CBP30), which restored lenalidomide response in XG1LenRes. This strategy also appeared to be more broadly applicable as SGC-CBP30 could re-sensitize two resistant HMCLs with low but detectable CRBN expression to lenalidomide, suggesting that targeting CBP/E300 is a promising approach to restore IMiD sensitivity in MM with detectable CRBN expression.

Published

2019

12. Glycan Isomer Identification Using Ultraviolet Photodissociation Initiated Radical Chemistry.

Author

Riggs DL, Hofmann J, Hahm HS, Seeberger PH, Pagel K, and Julian RR

Subjects

Chromatography, High Pressure Liquid, Isomerism, Photolysis radiation effects, Polysaccharides chemistry, Polysaccharides analysis, Tandem Mass Spectrometry, Ultraviolet Rays

Abstract

Glycans are fundamental biological macromolecules, yet despite their prevalence and recognized importance, a number of unique challenges hinder routine characterization. The multiplicity of OH groups in glycan monomers easily afford branched structures and alternate linkage sites, which can result in isomeric structures that differ by minute details. Herein, radical chemistry is employed in conjunction with mass spectrometry to enable rapid, accurate, and high throughput identification of a challenging series of closely related glycan isomers. The results are compared with analysis by collision-induced dissociation, higher-energy collisional dissociation, and ultraviolet photodissociation (UVPD) at 213 nm. In general, collision-based activation struggles to produce characteristic fragmentation patterns, while UVPD and radical-directed dissociation (RDD) can distinguish all isomers. In the case of RDD, structural differentiation derives from radical mobility and subsequent fragmentation. For glycans, the energetic landscape for radical migration is flat, increasing the importance of the three-dimensional structure. RDD is therefore a powerful and straightforward method for characterizing glycan isomers.

Published

2018

13. Sequence and Solution Effects on the Prevalence of d-Isomers Produced by Deamidation.

Author

Riggs DL, Gomez SV, and Julian RR

Subjects

Amino Acid Sequence, Buffers, Isomerism, Mass Spectrometry, Models, Molecular, Protein Processing, Post-Translational, Amides chemistry, Asparagine chemistry, Peptides chemistry

Abstract

Deamidation of asparagine is a spontaneous and irreversible post-translational modification associated with a growing list of human diseases. While pervasive, deamidation is often overlooked because it represents a relatively minor chemical change. Structural and functional characterization of this modification is complicated because deamidation of asparagine yields four isomeric forms of Asp. Herein, radical directed dissociation (RDD), in conjunction with mass spectrometry, is used to identify and quantify all four isomers in a series of model peptides that were subjected to various deamidation conditions. Although primary sequence significantly influences the rate of deamidation, it has little impact on the relative proportions of the product isomers. Furthermore, the addition of ammonia can be used to increase the rate of deamidation without significantly perturbing isomer populations. Conversely, external factors such as buffer conditions and temperature alter product distributions but exhibit less dramatic effects on the deamidation rate. Strikingly, the common laboratory and biologically significant bicarbonate buffer is found to strongly promote racemization, yielding increased amounts of d-Asp and d-isoAsp. These outcomes following deamidation have broad implications in human aging and should be considered during the development of protein-based therapeutics.

Published

2017

14. IAP antagonists induce anti-tumor immunity in multiple myeloma.

Author

Chesi M, Mirza NN, Garbitt VM, Sharik ME, Dueck AC, Asmann YW, Akhmetzyanova I, Kosiorek HE, Calcinotto A, Riggs DL, Keane N, Ahmann GJ, Morrison KM, Fonseca R, Lacy MQ, Dingli D, Kumar SK, Ailawadhi S, Dispenzieri A, Buadi F, Gertz MA, Reeder CB, Lin Y, Chanan-Khan AA, Stewart AK, Fooksman D, and Bergsagel PL

Subjects

Aged, Aged, 80 and over, Animals, Antineoplastic Agents pharmacology, Cell Line, Tumor, Cyclophosphamide pharmacology, Dendritic Cells drug effects, Dendritic Cells immunology, Disease Models, Animal, Female, Gene Expression drug effects, Humans, Interferon Type I drug effects, Interferon Type I immunology, Macrophages drug effects, Macrophages immunology, Male, Mice, Mice, Transgenic, Middle Aged, Multiple Myeloma immunology, Neoplasm Recurrence, Local immunology, Phagocytosis drug effects, Phagocytosis immunology, Thiazoles pharmacology, Antineoplastic Agents therapeutic use, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Multiple Myeloma drug therapy, Neoplasm Recurrence, Local drug therapy, Thiazoles therapeutic use

Abstract

The cellular inhibitors of apoptosis (cIAP) 1 and 2 are amplified in about 3% of cancers and have been identified in multiple malignancies as being potential therapeutic targets as a result of their role in the evasion of apoptosis. Consequently, small-molecule IAP antagonists, such as LCL161, have entered clinical trials for their ability to induce tumor necrosis factor (TNF)-mediated apoptosis of cancer cells. However, cIAP1 and cIAP2 are recurrently homozygously deleted in multiple myeloma (MM), resulting in constitutive activation of the noncanonical nuclear factor (NF)-κB pathway. To our surprise, we observed robust in vivo anti-myeloma activity of LCL161 in a transgenic myeloma mouse model and in patients with relapsed-refractory MM, where the addition of cyclophosphamide resulted in a median progression-free-survival of 10 months. This effect was not a result of direct induction of tumor cell death, but rather of upregulation of tumor-cell-autonomous type I interferon (IFN) signaling and a strong inflammatory response that resulted in the activation of macrophages and dendritic cells, leading to phagocytosis of tumor cells. Treatment of a MM mouse model with LCL161 established long-term anti-tumor protection and induced regression in a fraction of the mice. Notably, combination of LCL161 with the immune-checkpoint inhibitor anti-PD1 was curative in all of the treated mice.

Published

2016

15. A Novel Interaction between Pyk2 and MAP4K4 Is Integrated with Glioma Cell Migration.

Author

Loftus JC, Yang Z, Kloss J, Dhruv H, Tran NL, and Riggs DL

Abstract

Glioma cell migration correlates with Pyk2 activity, but the intrinsic mechanism that regulates the activity of Pyk2 is not fully understood. Previous studies have supported a role for the N-terminal FERM domain in the regulation of Pyk2 activity as mutations in the FERM domain inhibit Pyk2 phosphorylation. To search for novel protein-protein interactions mediated by the Pyk2 FERM domain, we utilized a yeast two-hybrid genetic selection to identify the mammalian Ste20 homolog MAP4K4 as a binding partner for the Pyk2 FERM domain. MAP4K4 coimmunoprecipitated with Pyk2 and was a substrate for Pyk2 but did not coimmunoprecipitate with the closely related focal adhesion kinase FAK. Knockdown of MAP4K4 expression inhibited glioma cell migration and effectively blocked Pyk2 stimulation of glioma cell. Increased expression of MAP4K4 stimulated glioma cell migration; however, this stimulation was blocked by knockdown of Pyk2 expression. These data support that the interaction of MAP4K4 and Pyk2 is integrated with glioma cell migration and suggest that inhibition of this interaction may represent a potential therapeutic strategy to limit glioblastoma tumor dispersion.

Published

2013

16. Targeting the regulation of androgen receptor signaling by the heat shock protein 90 cochaperone FKBP52 in prostate cancer cells.

Author

De Leon JT, Iwai A, Feau C, Garcia Y, Balsiger HA, Storer CL, Suro RM, Garza KM, Lee S, Kim YS, Chen Y, Ning YM, Riggs DL, Fletterick RJ, Guy RK, Trepel JB, Neckers LM, and Cox MB

Subjects

Animals, Cell Line, Tumor, Cell Proliferation drug effects, Drug Discovery, Enzyme-Linked Immunosorbent Assay, Fluorescence, Humans, Immunoblotting, Immunoprecipitation, Male, Mice, Molecular Dynamics Simulation, Molecular Structure, Receptors, Androgen chemistry, Tacrolimus Binding Proteins metabolism, Yeasts, beta-Galactosidase, Gene Expression Regulation drug effects, HSP90 Heat-Shock Proteins metabolism, Models, Molecular, Multiprotein Complexes metabolism, Prostatic Neoplasms metabolism, Receptors, Androgen metabolism, Tacrolimus Binding Proteins antagonists & inhibitors

Abstract

Drugs that target novel surfaces on the androgen receptor (AR) and/or novel AR regulatory mechanisms are promising alternatives for the treatment of castrate-resistant prostate cancer. The 52 kDa FK506 binding protein (FKBP52) is an important positive regulator of AR in cellular and whole animal models and represents an attractive target for the treatment of prostate cancer. We used a modified receptor-mediated reporter assay in yeast to screen a diversified natural compound library for inhibitors of FKBP52-enhanced AR function. The lead compound, termed MJC13, inhibits AR function by preventing hormone-dependent dissociation of the Hsp90-FKBP52-AR complex, which results in less hormone-bound receptor in the nucleus. Assays in early and late stage human prostate cancer cells demonstrated that MJC13 inhibits AR-dependent gene expression and androgen-stimulated prostate cancer cell proliferation.

Published

2011

17. FK506-binding protein 52 phosphorylation: a potential mechanism for regulating steroid hormone receptor activity.

Author

Cox MB, Riggs DL, Hessling M, Schumacher F, Buchner J, and Smith DF

Subjects

Amino Acid Sequence, Animals, Catalytic Domain, Circular Dichroism, HSP90 Heat-Shock Proteins metabolism, Humans, Mice, Models, Molecular, Molecular Sequence Data, Mutation genetics, Phosphorylation, Phosphothreonine metabolism, Protein Structure, Tertiary, Sequence Alignment, Sequence Homology, Amino Acid, Structural Homology, Protein, Tacrolimus Binding Proteins chemistry, Tacrolimus Binding Proteins genetics, Receptors, Steroid metabolism, Tacrolimus Binding Proteins metabolism

Abstract

Functional maturation of steroid hormone receptors requires ordered assembly into a large multichaperone complex consisting of receptor monomer, an Hsp90 dimer, the p23 cochaperone, and an FK506-binding protein (FKBP) family member or alternate peptidylprolyl isomerase-related cochaperone. Previous cellular studies demonstrated that FKBP52 can potentiate receptor function. These results have been confirmed in fkbp4 gene knockout mice in which males are partially androgen insensitive and females display characteristics of progesterone insensitivity. Conversely, FKBP51, which has a high degree of similarity to FKBP52, antagonizes FKBP52-mediated potentiation. Both proteins consist of three domains: two FKBP12-like domains termed FK1 and FK2 and a tetratricopeptide repeat domain that targets binding to Hsp90. To help understand why the two FKBPs behave differently and to gain insight into FKBP52 potentiation activity, we have analyzed the loop structure that links FK1 and FK2. Within the FK linker of FKBP52 is the sequence TEEED, which forms a consensus casein kinase II phosphorylation site; the corresponding sequence in FKBP51 is FED. We demonstrate that the distinct FK linker sequences per se do not account for lack of potentiation activity by FKBP51. However, phosphorylation of the FK linker appears to be an important regulatory determinant of FKBP52-mediated potentiation of steroid receptor activity.

Published

2007

18. Noncatalytic role of the FKBP52 peptidyl-prolyl isomerase domain in the regulation of steroid hormone signaling.

Author

Riggs DL, Cox MB, Tardif HL, Hessling M, Buchner J, and Smith DF

Subjects

Amino Acid Sequence, Animals, Catalysis, Drug Synergism, Mice, Models, Molecular, Molecular Sequence Data, Mutant Proteins isolation & purification, Mutant Proteins metabolism, Mutation genetics, Protein Structure, Tertiary, Recombinant Fusion Proteins metabolism, Selection, Genetic, Structure-Activity Relationship, Peptidylprolyl Isomerase chemistry, Signal Transduction drug effects, Steroids pharmacology, Tacrolimus Binding Proteins chemistry, Tacrolimus Binding Proteins metabolism

Abstract

Hormone-dependent transactivation by several of the steroid hormone receptors is potentiated by the Hsp90-associated cochaperone FKBP52, although not by the closely related FKBP51. Here we analyze the mechanisms of potentiation and the functional differences between FKBP51 and FKBP52. While both have peptidyl-prolyl isomerase activity, this is not required for potentiation, as mutations abolishing isomerase activity did not affect potentiation. Genetic selection in Saccharomyces cerevisiae for gain of potentiation activity in a library of randomly mutated FKBP51 genes identified a single residue at position 119 in the N-terminal FK1 domain as being a critical difference between these two proteins. In both the yeast model and mammalian cells, the FKBP51 mutation L119P, which is located in a hairpin loop overhanging the catalytic pocket and introduces the proline found in FKBP52, conferred significant potentiation activity, whereas the converse P119L mutation in FKBP52 decreased potentiation. A second residue in this loop, A116, also influences potentiation levels; in fact, the FKBP51-A116V L119P double mutant potentiated hormone signaling as well as wild-type FKBP52 did. These results suggest that the FK1 domain, and in particular the loop overhanging the catalytic pocket, is critically involved in receptor interactions and receptor activity.

Published

2007

19. Physiological role for the cochaperone FKBP52 in androgen receptor signaling.

Author

Cheung-Flynn J, Prapapanich V, Cox MB, Riggs DL, Suarez-Quian C, and Smith DF

Subjects

Animals, Blotting, Western, Dose-Response Relationship, Drug, Gene Deletion, Genetic Vectors, Genotype, HSP90 Heat-Shock Proteins metabolism, Humans, Immunohistochemistry, Male, Mice, Mice, Knockout, Models, Genetic, Models, Molecular, Molecular Chaperones, Plasmids metabolism, Point Mutation, Proline chemistry, Prostate metabolism, Protein Binding, Protein Conformation, Protein Folding, Protein Structure, Tertiary, Receptors, Androgen chemistry, Signal Transduction, Testis metabolism, Tissue Distribution, Transcriptional Activation, Receptors, Androgen metabolism, Tacrolimus Binding Proteins genetics, Tacrolimus Binding Proteins physiology

Abstract

Molecular chaperones mediate multiple aspects of steroid receptor function, but the physiological importance of most receptor-associated cochaperones has not been determined. To help fill this gap, we targeted for disruption the mouse gene for the 52-kDa FK506 binding protein, FKBP52, a 90-kDa heat shock protein (Hsp90)-binding immunophilin found in steroid receptor complexes. A mouse line lacking FKBP52 (52KO) was generated and characterized. Male 52KO mice have several defects in reproductive tissues consistent with androgen insensitivity; among these defects are ambiguous external genitalia and dysgenic prostate. FKBP52 and androgen receptor (AR) are coexpressed in prostate epithelial cells of wild-type mice. However, FKBP52 and AR are similarly coexpressed in testis even though testis morphology and spermatogenesis in 52KO males are usually normal. Molecular studies confirm that FKBP52 is a component of AR complexes, and cellular studies in yeast and human cell models demonstrate that FKBP52 can enhance AR-mediated transactivation. AR enhancement requires FKBP52 peptidylprolyl isomerase activity as well as Hsp90-binding ability, and enhancement probably relates to an affect of FKBP52 on AR-folding pathways. In the presence of FKBP52, but not other cochaperones, the function of a minimally active AR point mutant can be dramatically restored. We conclude that FKBP52 is an AR folding factor that has critically important physiological roles in some male reproductive tissues.

Published

2005

20. Functional comparison of human and Drosophila Hop reveals novel role in steroid receptor maturation.

Author

Carrigan PE, Riggs DL, Chinkers M, and Smith DF

Subjects

Adaptor Proteins, Vesicular Transport metabolism, Amino Acid Sequence, Animals, Cloning, Molecular, Drosophila Proteins, HSP70 Heat-Shock Proteins metabolism, HSP90 Heat-Shock Proteins metabolism, Heat-Shock Proteins physiology, Heterotrimeric GTP-Binding Proteins, Humans, Janus Kinases, Mice, Molecular Sequence Data, Protein-Tyrosine Kinases physiology, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins metabolism, Saccharomyces cerevisiae genetics, Sequence Alignment, Sequence Homology, Amino Acid, Transcription Factors, Drosophila physiology, Heat-Shock Proteins chemistry, Protein-Tyrosine Kinases chemistry, Receptors, Glucocorticoid physiology, Receptors, Steroid physiology

Abstract

Hsp70/Hsp90 organizing protein (Hop) coordinates Hsp70 and Hsp90 interactions during assembly of steroid receptor complexes. Hop is composed of three tetratricopeptide repeat (TPR) domains (TPR1, TPR2a, and TPR2b) and two DP repeat domains (DP1 and DP2); Hsp70 interacts directly with TPR1 and Hsp90 with TPR2a, but the function of other domains is less clear. Human Hop and the Saccharomyces cerevisiae ortholog Sti1p, which share a common domain arrangement, are functionally interchangeable in a yeast growth assay and in supporting the efficient maturation of glucocorticoid receptor (GR) function. To gain a better understanding of Hop structure/function relationships, we have extended comparisons to the Hop ortholog from Drosophila melanogaster (dHop), which lacks DP1. Although dHop binds Hsp70 and Hsp90 and can rescue the growth defect in yeast lacking Sti1p, dHop failed to support GR function in yeast, which suggests a novel role for Hop in GR maturation that goes beyond Hsp binding. Chimeric Hop constructs combining human and Drosophila domains demonstrate that the C-terminal domain DP2 is critical for this previously unrecognized role in steroid receptor function.

Published

2005

21. Functional specificity of co-chaperone interactions with Hsp90 client proteins.

Author

Riggs DL, Cox MB, Cheung-Flynn J, Prapapanich V, Carrigan PE, and Smith DF

Subjects

Animals, Cell Cycle Proteins metabolism, Chaperonins, Drosophila Proteins metabolism, Humans, Immunophilins metabolism, Intracellular Signaling Peptides and Proteins, Molecular Chaperones metabolism, Proteins chemistry, Proteins metabolism, Substrate Specificity, HSP90 Heat-Shock Proteins metabolism

Abstract

A wide array of proteins in signal transduction pathways depend on Hsp90 and other chaperone components for functional maturation, regulation, and stability. Among these Hsp90 client proteins are steroid receptors, members from other classes of transcription factors, and representatives of both serine/threonine and tyrosine kinase families. Typically, dynamic complexes form on the client protein, and these consist of Hsp90- plus bound co-chaperones that often have enzymatic activities. In addition to its direct influence on client folding, Hsp90 locally concentrates co-chaperone activity within the client complex, and dynamic exchange of co-chaperones on Hsp90 facilitates sampling of co-chaperone activities that may, or may not, act on the client protein. We are just beginning to understand the nature of biochemical and molecular interactions between co-chaperone and Hsp90-bound client. This review focuses on the differential effects of Hsp90 co-chaperones toward client protein function and on the specificity that allows co-chaperones to discriminate between even closely related clients.

Published

2004

22. The heat shock protein 70 cochaperone hip enhances functional maturation of glucocorticoid receptor.

Author

Nelson GM, Prapapanich V, Carrigan PE, Roberts PJ, Riggs DL, and Smith DF

Subjects

Animals, Carrier Proteins genetics, Estradiol pharmacology, HSP70 Heat-Shock Proteins genetics, Heat-Shock Proteins genetics, Heat-Shock Proteins metabolism, Humans, Molecular Chaperones genetics, Molecular Chaperones metabolism, Progesterone pharmacology, Rats, Receptors, Glucocorticoid drug effects, Receptors, Glucocorticoid genetics, Temperature, Transcriptional Activation, Tumor Suppressor Proteins genetics, Yeasts genetics, Yeasts growth & development, Yeasts metabolism, Carrier Proteins metabolism, HSP70 Heat-Shock Proteins metabolism, Receptors, Glucocorticoid metabolism, Tumor Suppressor Proteins metabolism

Abstract

Multiple molecular chaperones interact with steroid receptors to promote functional maturation and stability of receptor complexes. The heat shock protein (Hsp)70 cochaperone Hip has been identified in conjunction with Hsp70, Hsp90, and the Hsp70/Hsp90 cochaperone Hop/Sti1p in receptor complexes during an intermediate stage of receptor assembly, but a functional requirement for Hip in the receptor assembly process has not been established. Because the budding yeast Saccharomyces cerevisiae contains orthologs for most of the receptor-associated chaperones yet lacks an orthologous Hip gene, we exploited the well-established yeast model for steroid receptor function to ask whether Hip can alter steroid receptor function in vivo. Introducing human Hip into yeast enhances hormone-dependent activation of a reporter gene by glucocorticoid receptor (GR). Because Hip does not similarly enhance signaling by mineralocorticoid, progesterone, or estrogen receptors, a general effect on transcription can be excluded. Instead, Hip promotes functional maturation of GR without increasing steady-state levels of GR protein. Unexpectedly, Hip binding to Hsp70 is not critical for boosting GR responsiveness to hormone. In conclusion, Hip functions by a previously unrecognized mechanism to promote the efficiency of GR maturation in cells.

Published

2004

23. Multiple domains of the co-chaperone Hop are important for Hsp70 binding.

Author

Carrigan PE, Nelson GM, Roberts PJ, Stoffer J, Riggs DL, and Smith DF

Subjects

Amino Acid Motifs, Amino Acid Sequence, Animals, Binding Sites, Circular Dichroism, HSP70 Heat-Shock Proteins genetics, HSP70 Heat-Shock Proteins metabolism, HSP90 Heat-Shock Proteins genetics, HSP90 Heat-Shock Proteins metabolism, Humans, Kinetics, Molecular Chaperones chemistry, Molecular Chaperones genetics, Molecular Chaperones metabolism, Molecular Sequence Data, Protein Binding, Protein Folding, Protein Structure, Tertiary, Rats, Repetitive Sequences, Nucleic Acid, HSP70 Heat-Shock Proteins chemistry, HSP90 Heat-Shock Proteins chemistry

Abstract

The Hop/Sti1 co-chaperone binds to both Hsp70 and Hsp90. Biochemical and co-crystallographic studies have suggested that the EEVD-containing C terminus of Hsp70 or Hsp90 binds specifically to one of the Hop tetratricopeptide repeat domains, TPR1 or TPR2a, respectively. Mutational analyses of Hsp70 and Hop were undertaken to better characterize interactions between the C terminus of Hsp70 and Hop domains. Surprisingly, truncation of EEVD plus as many as 34 additional amino acids from the Hsp70 C terminus did not reduce the ability of Hsp70 mutants to co-immunoprecipitate with Hop, although further truncation eliminated Hop binding. Hop point mutations targeting a carboxylate clamp position in TPR1 disrupted Hsp70 binding, as was expected; however, similar point mutations in TPR2a or TPR2b also inhibited Hsp70 binding in some settings. Using a yeast-based in vivo assay for Hop function, wild type Hop and TPR2b mutants could fully complement deletion of Sti1p; TPR1 and TPR2a point mutants could partially restore activity. Conformations of Hop and Hop mutants were probed by limited proteolysis. The TPR1 mutant digested in a similar manner to wild type; however, TPR2a and TPR2b mutants each displayed greater resistance to chymotryptic digestion. All point mutants retained an ability to dimerize, and none appeared to be grossly misfolded. These results raise questions about current models for Hop/Hsp70 interaction.

Published

2004

24. Direct-to-consumer advertising: developing evidence-based policy to improve retention and comprehension.

Author

Riggs DL, Holdsworth SM, and McAvoy DR

Subjects

Drug Industry, Humans, Policy Making, United States, Advertising methods, Community Participation, Evidence-Based Medicine, Pharmaceutical Preparations

Abstract

Pharmaceutical advertising was historically directed toward health care professionals and mainly communicated through medical journals. The arrival of direct-to-consumer advertising has sparked both praise and criticism. Although current Food and Drug Administration requirements for drug promotion were written from a health care professional perspective, the same regulations have been applied to advertising directed at consumers. This has led to questions regarding the appropriate method for communicating detailed medical information. Rigorous research is needed to evaluate and determine the most effective format for communicating benefit and risk information to consumers. New standards for drug advertising to consumers should be grounded in data derived from this type of research.

Published

2004

25. C-terminal sequences outside the tetratricopeptide repeat domain of FKBP51 and FKBP52 cause differential binding to Hsp90.

Author

Cheung-Flynn J, Roberts PJ, Riggs DL, and Smith DF

Subjects

Amino Acid Sequence, Binding Sites genetics, Humans, Molecular Sequence Data, Protein Binding, Recombinant Proteins genetics, Recombinant Proteins metabolism, Repetitive Sequences, Nucleic Acid, Sequence Analysis, Tacrolimus Binding Proteins genetics, HSP90 Heat-Shock Proteins metabolism, Tacrolimus Binding Proteins metabolism

Abstract

Hsp90 assembles with steroid receptors and other client proteins in association with one or more Hsp90-binding cochaperones, some of which contain a common tetratricopeptide repeat (TPR) domain. Included in the TPR cochaperones are the Hsp70-Hsp90-organizing protein Hop, the FK506-binding immunophilins FKBP52 and FKBP51, the cyclosporin A-binding immunophilin CyP40, and protein phosphatase PP5. The TPR domains from these proteins have similar x-ray crystallographic structures and target cochaperone binding to the MEEVD sequence that terminates Hsp90. However, despite these similarities, the TPR cochaperones have distinctive properties for binding Hsp90 and assembling with Hsp90.steroid receptor complexes. To identify structural features that differentiate binding of FKBP51 and FKBP52 to Hsp90, we generated an assortment of truncation mutants and chimeras that were compared for coimmunoprecipitation with Hsp90. Although the core TPR domain (approximately amino acids 260-400) of FKBP51 and FKBP52 is required for Hsp90 binding, the C-terminal 60 amino acids (approximately 400-end) also influence Hsp90 binding. More specifically, we find that amino acids 400-420 play a critical role for Hsp90 binding by either FKBP. Within this 20-amino acid region, we have identified a consensus sequence motif that is also present in some other TPR cochaperones. Additionally, the final 30 amino acids of FKBP51 enhance binding to Hsp90, whereas the corresponding region of FKBP52 moderates binding to Hsp90. Taking into account the x-ray crystal structure for FKBP51, we conclude that the C-terminal regions of FKBP51 and FKBP52 outside the core TPR domains are likely to assume alternative conformations that significantly impact Hsp90 binding.

Published

2003

26. The Hsp90-binding peptidylprolyl isomerase FKBP52 potentiates glucocorticoid signaling in vivo.

Author

Riggs DL, Roberts PJ, Chirillo SC, Cheung-Flynn J, Prapapanich V, Ratajczak T, Gaber R, Picard D, and Smith DF

Subjects

Animals, Dose-Response Relationship, Drug, Gene Expression Regulation, Genes, Reporter, Humans, Models, Molecular, Molecular Chaperones genetics, Molecular Chaperones metabolism, Protein Binding, Protein Conformation, Receptors, Glucocorticoid metabolism, Saccharomyces cerevisiae physiology, Transcriptional Activation, Glucocorticoids metabolism, HSP90 Heat-Shock Proteins metabolism, Peptidylprolyl Isomerase metabolism, Signal Transduction physiology, Tacrolimus Binding Proteins metabolism

Abstract

Hsp90 is required for the normal activity of steroid receptors, and in steroid receptor complexes it is typically bound to one of the immunophilin-related co-chaperones: the peptidylprolyl isomerases FKBP51, FKBP52 or CyP40, or the protein phosphatase PP5. The physiological roles of the immunophilins in regulating steroid receptor function have not been well defined, and so we examined in vivo the influences of immunophilins on hormone-dependent gene activation in the Saccharomyces cerevisiae model for glucocorticoid receptor (GR) function. FKBP52 selectively potentiates hormone-dependent reporter gene activation by as much as 20-fold at limiting hormone concentrations, and this potentiation is readily blocked by co-expression of the closely related FKBP51. The mechanism for potentiation is an increase in GR hormone-binding affinity that requires both the Hsp90-binding ability and the prolyl isomerase activity of FKBP52.

Published

2003

27. Probing the environment of nascent RNA in Escherichia coli transcription elongation complexes utilizing a new fluorescent ribonucleotide analog.

Author

Hanna MM, Yuriev E, Zhang J, and Riggs DL

Subjects

Base Sequence, DNA chemistry, DNA-Directed RNA Polymerases metabolism, Escherichia coli enzymology, Fluorescence Polarization, Fluorescent Dyes chemical synthesis, Fluorescent Dyes chemistry, Models, Molecular, Molecular Structure, Nucleic Acid Hybridization, RNA Probes chemical synthesis, Transcription, Genetic, Uridine Triphosphate chemical synthesis, Uridine Triphosphate chemistry, Escherichia coli genetics, RNA Probes chemistry, Transcription Factors genetics, Uridine Triphosphate analogs & derivatives

Abstract

We report the synthesis and characterization of 5-thioacetamidofluorescein-uridine 5'-triphosphate (5-SF-UTP), and its application to the characterization of the environment of the nascent RNA during trans-cription. This analog specifically replaced UTP as a transcription substrate for Escherichia coli and T7 RNA polymerases, and yeast RNA polymerase III. Escherichia coli transcription complexes containing analog incorporated at only position +21 of the RNA were prepared. The RNA was then elongated in the absence of analog, moving the fluorescent group further away from the enzyme active site, and the fluorescence polarization was measured. Analog positioned near the 3' end of the transcript exhibited significantly increased polarization relative to that of free probe, consistent with the constrained environment of the RNA in the DNA-RNA hybrid. Analog positioned 14 nucleotides from the 3' end exhibited significantly decreased polarization relative to that at the 3' end of the RNA, but only slightly above that of free RNA, suggesting that the probe was on the solvent-exposed surface of the polymerase. Molecular modeling of these analog-substituted RNAs produced structures consistent with the experimental data. The excellent substrate properties of this analog make it useful for the characterization of the environment of RNA not only during transcription and translation, but in any type of ribonucleoprotein complex.

Published

1999

28. Regulation of the RNA polymerase I and III transcription systems in response to growth conditions.

Author

Clarke EM, Peterson CL, Brainard AV, and Riggs DL

Subjects

Cell Cycle, Cell Division, Cells, Cultured, DNA Footprinting, In Vitro Techniques, Plasmids metabolism, RNA biosynthesis, RNA, Ribosomal, 5S biosynthesis, Yeasts, RNA Polymerase I metabolism, RNA Polymerase III metabolism, Transcription, Genetic

Abstract

To better understand the mechanisms that regulate stable RNA synthesis, we have analyzed the RNA polymerase I and III transcriptional activities of extracts isolated from cells propagated under a variety of conditions. Under balanced growth conditions the levels of both RNA polymerase I- and III-specific transcription increased proportionally with growth rate. Upon nutritional starvation, RNA polymerase I transcription rapidly declined, followed by 5 S rDNA and eventually tDNA transcription. Transcriptional activities in extracts were restored when the nongrowing cultures were resuspended in fresh medium, although growth did not resume. The differential expression of 5 S rDNA and tDNA genes in extracts prepared from cells subjected to partial starvation was traced to a 5 S rDNA-specific inhibitor and not to a defect in any RNA polymerase III transcription factor. Characterization of this inhibitor indicated that it was not 5 S rRNA. It was sensitive to phenol extraction and resistant to RNase, and its target did not appear to be transcription factor IIIA. Not all treatments that slowed or stopped growth down-regulated the stable RNA transcription apparatus. Cells that have been subjected to either energy starvation or cycloheximide treatment still retain the ability to synthesize stable RNA in vitro, suggesting the presence of alternative regulatory mechanisms.

Published

1996

29. Preparation of probe-modified RNA with 5-mercapto-UTP for analysis of protein-RNA interactions.

Author

He B, Riggs DL, and Hanna MM

Subjects

Base Sequence, Cross-Linking Reagents, DNA-Directed RNA Polymerases metabolism, Escherichia coli genetics, Escherichia coli metabolism, Hydrogen-Ion Concentration, In Vitro Techniques, Molecular Sequence Data, Photochemistry, Protein Binding, RNA chemistry, RNA genetics, RNA Probes chemical synthesis, RNA Probes chemistry, RNA Probes genetics, RNA Processing, Post-Transcriptional, RNA, Bacterial chemistry, RNA, Bacterial genetics, RNA, Bacterial metabolism, RNA-Binding Proteins metabolism, Substrate Specificity, Uridine Triphosphate chemical synthesis, RNA chemical synthesis, Thionucleotides chemical synthesis, Uridine Triphosphate analogs & derivatives

Abstract

We report a modified synthesis for 5-mercapto-UTP (5-SH-UTP) and its use for analysis of protein-RNA interactions utilizing Escherichia coli and T7 RNA polymerases and yeast RNA polymerases I and III. 5-SH-UTP did not affect transcriptional pausing, Rho-independent termination or recognition of the E. coli transcription complex by NusA. RNA containing 5-SH-UMP did not crosslink to polymerase when irradiation was 302 or 337 nm. Transcription complexes containing RNA substituted with 5-SH-UMP were post-transcriptionally modified to attach a photocross-linking group to thiol-tagged nucleotides in the RNA on the surface of the polymerase of free in solution. The pKa for 5-SH-UTP was determined to be 5.6, so modification of the thiol groups in the RNA with p-azidophenacyl bromide could be carried out at pH 7. Addition of the transcription termination factor Rho, a RNA binding protein, to E. coli transcription complexes resulted in RNA crosslinking to Rho and to the beta and beta' subunits of polymerase. Using 5-SH-UTP, one can distinguish RNA binding domains on the surface of RNA polymerases or other RNA binding proteins from those buried within the protein.

Published

1995

30. Characterization of the components of reconstituted Saccharomyces cerevisiae RNA polymerase I transcription complexes.

Author

Riggs DL, Peterson CL, Wickham JQ, Miller LM, Clarke EM, Crowell JA, and Sergere JC

Subjects

Chromatography, Ion Exchange, DNA, Ribosomal metabolism, DNA-Binding Proteins isolation & purification, DNA-Binding Proteins metabolism, Plasmids, RNA Polymerase I isolation & purification, Restriction Mapping, Saccharomyces cerevisiae growth & development, TATA Box, Transcription Factors isolation & purification, Ultracentrifugation, RNA Polymerase I metabolism, Saccharomyces cerevisiae metabolism, Transcription Factors metabolism, Transcription, Genetic

Abstract

We have reconstituted specific RNA polymerase I transcription from three partially purified chromatographic fractions (termed A, B, and C). Here, we present the chromatographic scheme and the initial biochemical characterization of these fractions. The A fraction contained the RNA polymerase I transcription factor(s), which was necessary and sufficient to form stable preinitiation complexes at the promoter. Of the three fractions, only fraction A contained a significant amount of the TATA binding factor. The B fraction contributed RNA polymerase I, and it contained an essential RNA polymerase I transcription factor that was specifically inactivated in response to a significant decrease in growth rate. The function of the C fraction remains unclear. This reconstituted transcription system provides a starting point for the biochemical dissection of the yeast RNA polymerase I transcription complex, thus allowing in vitro experiments designed to elucidate the molecular mechanisms controlling rRNA synthesis.

Published

1995

31. The yeast RNA polymerase I promoter: ribosomal DNA sequences involved in transcription initiation and complex formation in vitro.

Author

Kulkens T, Riggs DL, Heck JD, Planta RJ, and Nomura M

Subjects

Base Sequence, DNA, Fungal genetics, Escherichia coli metabolism, Macromolecular Substances, Molecular Sequence Data, Mutation genetics, Saccharomyces cerevisiae genetics, Transcription, Genetic genetics, DNA, Ribosomal genetics, Genes, Fungal, Promoter Regions, Genetic genetics, RNA Polymerase I genetics, Saccharomyces cerevisiae enzymology

Abstract

Using an in vitro transcription system for Saccharomyces cerevisiae RNA polymerase I, we have analyzed Pol I promoter deletion mutants and mapped the boundaries of the promoter between positions -155 and +27. The 5'-boundary of the minimal core promoter capable of transcription initiation, however, was found to lie between -38 and -26. The 3'-deletion extending to -2 and -5 still allowed some transcription, suggesting that the positioning of Pol I is directed by upstream sequences. The results of in vitro analysis of linker scanning mutants (LSMs) combined with the deletion analysis showed that the promoter consists of three domains: two essential core domains (I: -28 to +8 and II: -76 to -51) and a transcription modulating upstream domain (III: -146 to -91). These results are in general agreement with those obtained in vivo (1). Using a template competition assay we also analyzed these mutant promoters for their ability to form a stable preinitiation complex. We found that the ability of 5'-deletion mutants to sequester an essential factor(s) correlates with their transcriptional activity. In contrast, several 3'-deletions and some LSMs in domain I and II decrease transcription activity greatly without significantly decreasing competition ability. The results indicate that the stimulatory function of domain III is achieved through its interaction with an essential transcription factor(s), although the other domains also participate in this interaction, perhaps directly or through another protein factor.

Published

1991

32. Specific transcription of Saccharomyces cerevisiae 35 S rDNA by RNA polymerase I in vitro.

Author

Riggs DL and Nomura M

Subjects

Base Sequence, Chromosome Mapping, Macromolecular Substances, Molecular Sequence Data, Plasmids, RNA Polymerase III metabolism, Saccharomyces cerevisiae enzymology, Saccharomyces cerevisiae growth & development, Templates, Genetic, DNA, Ribosomal genetics, RNA Polymerase I metabolism, RNA, Ribosomal genetics, Saccharomyces cerevisiae genetics, Transcription, Genetic

Abstract

Specific transcription of yeast 35 S rDNA by RNA polymerase I has been demonstrated using fractionated extracts prepared from whole cells of Saccharomyces cerevisiae. Determination of the 5'-nucleotides of the in vitro transcripts indicated that two apparent start sites, corresponding to the first (initiating) and fifth nucleotide of the in vivo transcript, were utilized. Production of the 35 S rDNA transcript in this system was not inhibited by alpha-amanitin. Specific transcription of both the 35 S and 5 S rDNA sequences contained on the same template occurred simultaneously in these extracts. Sequential template competition experiments demonstrated that 35 S and 5 S rDNA transcription required different transcription factors. Specific antisera raised against the largest subunit of RNA polymerase I significantly inhibited synthesis of the 35 S rDNA transcript, but had a negligible effect on 5 S rRNA synthesis by RNA polymerase III. Additionally, this 35 S rDNA transcriptional activity was present in extracts prepared from a strain deficient in the mitochondrial RNA polymerase. Experiments using truncated rDNA templates showed that in vitro no more than 206 base pairs of the sequence upstream of the initiation site are required for maximal activity in this system; the enhancer element did not stimulate 35 S rDNA transcription.

Published

1990

33. Evidence of a second nitrate reductase activity that is distinct from the respiratory enzyme in Salmonella typhimurium.

Author

Barrett EL and Riggs DL

Subjects

Chlorates pharmacology, Chromosome Mapping, Chromosomes, Bacterial, Cytochromes biosynthesis, Genes, Bacterial, Mutation, Nitrate Reductases genetics, Nitrates metabolism, Nitrite Reductases metabolism, Salmonella typhimurium drug effects, Salmonella typhimurium genetics, Nitrate Reductases metabolism, Salmonella typhimurium enzymology

Abstract

Significant nitrate reductase activity was detected in mutants of Salmonella typhimurium which mapped at or near chlC and which were incapable of growth with nitrate as electron acceptor. The same mutants were sensitive to chlorate and performed sufficient nitrate reduction to permit anaerobic growth with nitrate as the sole nitrogen source in media containing glucose. The mutant nitrate-reducing protein did not migrate with the wild-type nitrate reductase in polyacrylamide electrophoretic gels. Studies of the electrophoretic mobility in gels of different polyacrylamide concentration revealed that the wild-type and mutant nitrate reductases differed significantly in both size and charge. The second enzyme also differed from the wild-type major enzyme in its response to repression by low pH and its lack of response to repression by glucose. The same mutants were found to be derepressed for nitrite reductase and for a cytochrome with a maximal reduced absorbance at 555 nm at 25 degrees C. This cytochrome was not detected in preparations of the wild type grown under the same conditions. Extracts of these mutants contained normal amounts of the b-type cytochromes which, in the wild type, were associated with nitrate reductase and formate dehydrogenase, respectively, although they could not mediate the oxidation of these cytochromes with nitrate. They were capable of oxidizing the derepressed 555-nm peak cytochrome with nitrate. It is suggested that these mutants synthesize a nitrate-reducing enzyme which is distinct from the chlC gene product and which is repressed in the wild type during anaerobic growth with nitrate.

Published

1982

34. Correlation between histidine operon expression and guanosine 5'-diphosphate-3'-diphosphate levels during amino acid downshift in stringent and relaxed strains of Salmonella typhimurium.

Author

Shand RF, Blum PH, Mueller RD, Riggs DL, and Artz SW

Subjects

Genotype, Kinetics, Mutation, Promoter Regions, Genetic, Salmonella typhimurium drug effects, Salmonella typhimurium growth & development, Serine analogs & derivatives, Serine pharmacology, Species Specificity, Amino Acids metabolism, Guanine Nucleotides metabolism, Guanosine Tetraphosphate metabolism, Histidine biosynthesis, Operon, Salmonella typhimurium genetics

Abstract

We have analyzed the correlation of attenuator-independent expression of the Salmonella typhimurium histidine operon in vivo with levels of the "alarmone" guanosine 5'-diphosphate 3'-diphosphate. Amino acid downshift caused by serine hydroxamate addition increased his expression in a relA+ strain and decreased his expression in a relA mutant, whereas levels of guanosine 5'-diphosphate-3'-diphosphate varied in parallel with the changes in his expression in the two strains. In several experiments, overall variations in his expression ranged from 20- to 60-fold after downshift. The mild downshift allowed growth of the cultures to continue at near-preshift rates. Serine hydroxamate addition was also used to analyze the effect of amino acid downshift on induced expression of wild-type and mutant lac promoters. There was a 12-fold difference in lac expression when a relA+-relA1 pair was subjected to mild starvation but only a 3-fold difference when the strains carried the lacZpL8UV5 promoter mutation. These results suggest that guanosine 5'-diphosphate-3'-diphosphate stimulates gene expression in vivo at the level of transcription initiation.

Published

1989

35. Salmonella typhimurium mutants defective in the formate dehydrogenase linked to nitrate reductase.

Author

Barrett EL and Riggs DL

Subjects

Ascorbic Acid metabolism, Chromosome Mapping, Chromosomes, Bacterial, Cytochromes metabolism, Formate Dehydrogenases genetics, Mutation, Nitrate Reductases metabolism, Salmonella typhimurium genetics, Aldehyde Oxidoreductases metabolism, Cytochrome b Group, Formate Dehydrogenases metabolism, Photosystem II Protein Complex, Salmonella typhimurium enzymology

Abstract

Six fdn mutants of Salmonella typhimurium defective in the formation of nitrate reductase-linked formate dehydrogenase (FDHN) but capable of producing both the hydrogenase-linked formate dehydrogenase (FDHH) and nitrate reductase were characterized. Results of phage P22 transduction experiments indicated that there may be three fdn genes located on the metE-metB chromosomal segment and distinct from all previously identified fdh and chl loci. All six FDHH+ FDHN- mutants were found to make FDHN enzyme protein which was indistinguishable from that of the wild type in electrophoretic studies. However, the results of the spectral studies indicated that all six mutants were defective in the anaerobic cytochrome b559 associated with FDHN. All contained the cytochrome b559 associated with nitrate reductase in amounts equal to or greater than the wild type. The results of the transduction experiments also indicated that the metE- metB segment of the Salmonella chromosome resembles that of Escherichia coli more than was originally thought.

Published

1982

36. Promoter domain mediates guanosine tetraphosphate activation of the histidine operon.

Author

Riggs DL, Mueller RD, Kwan HS, and Artz SW

Subjects

DNA, Bacterial genetics, DNA, Superhelical genetics, Gene Expression Regulation, Transcription, Genetic drug effects, Guanine Nucleotides pharmacology, Guanosine Tetraphosphate pharmacology, Histidine genetics, Operon, Promoter Regions, Genetic, Salmonella typhimurium genetics

Abstract

We have analyzed the effects of the "alarmone" guanosine 5'-diphosphate 3'-diphosphate (ppGpp) on regulation of the Salmonella typhimurium histidine operon in vitro. Expression of the wild-type promoter, measured in a DNA-dependent transcription-translation system, was strongly dependent on ppGpp; addition of ppGpp stimulated his expression 22-fold with plasmid DNA templates. Oligonucleotide-directed, site-specific mutations that increase the homology of the -10 hexamer to the consensus sequence of the E sigma 70 promoters dramatically increased his expression in the absence of ppGpp and reduced the stimulation to less than a factor of 2. A deletion mutation that alters the sequence between the -10 hexamer and the start point of transcription, generated by BAL-31 nuclease, affected ppGpp regulation in a similar manner. We propose that the -10 hexamer sequence and the adjacent downstream region are both important in regulating transcription by ppGpp. Mechanisms to account for activation and repression of transcription by ppGpp are discussed.

Published

1986

37. Multiple states of protein-DNA interaction in the assembly of transcription complexes on Saccharomyces cerevisiae 5S ribosomal RNA genes.

Author

Braun BR, Riggs DL, Kassavetis GA, and Geiduschek EP

Subjects

Deoxyribonucleoproteins physiology, In Vitro Techniques, Macromolecular Substances, Promoter Regions, Genetic, Regulatory Sequences, Nucleic Acid, DNA, Ribosomal genetics, DNA-Binding Proteins physiology, RNA, Ribosomal genetics, RNA, Ribosomal, 5S genetics, Saccharomyces cerevisiae physiology, Transcription Factors physiology, Transcription, Genetic

Abstract

Multiple stages of protein-DNA interaction in the assembly of RNA polymerase III transcription complexes on a Saccharomyces cerevisiae 5S rRNA gene have been distinguished by DNase I "footprinting" and gel retardation. Transcription factor IIIA interacts with approximately 35 base pairs of the internal promoter region. Transcription factors IIIC and IIIB incrementally extend the interaction along the 5S gene, if, and only if, transcription factor IIIA is also bound. Complexes assembled from the complete set of purified transcription factors or from a complete transcription system extend over the entire transcription unit together with almost 50 base pairs of 5' flanking sequence.

Published

1989

38. Transcription factor IIIB generates extended DNA interactions in RNA polymerase III transcription complexes on tRNA genes.

Author

Kassavetis GA, Riggs DL, Negri R, Nguyen LH, and Geiduschek EP

Subjects

Base Sequence, Chromatography, Affinity, DNA, Fungal genetics, Deoxyribonuclease I, Fungal Proteins genetics, Fungal Proteins metabolism, Molecular Sequence Data, Plasmids, Protein Binding, Saccharomyces cerevisiae enzymology, Transcription Factor TFIIIB, Transcription Factors isolation & purification, Transcription, Genetic, Triazines, DNA, Fungal metabolism, DNA-Directed RNA Polymerases metabolism, RNA Polymerase III metabolism, RNA, Fungal genetics, RNA, Transfer genetics, Saccharomyces cerevisiae genetics, Transcription Factors metabolism, Transcription Factors, TFIII

Abstract

Transcription complexes that assemble on tRNA genes in a crude Saccharomyces cerevisiae cell extract extend over the entire transcription unit and approximately 40 base pairs of contiguous 5'-flanking DNA. We show here that the interaction with 5'-flanking DNA is due to a protein that copurifies with transcription factor TFIIIB through several steps of purification and shares characteristic properties that are normally ascribed to TFIIIB: dependence on prior binding of TFIIIC and great stability once the TFIIIC-TFIIIB-DNA complex is formed. SUP4 gene (tRNATyr) DNA that was cut within the 5'-flanking sequence (either 31 or 28 base pairs upstream of the transcriptional start site) was no longer able to stably incorporate TFIIIB into a transcription complex. The TFIIIB-dependent 5'-flanking DNA protein interaction was predominantly not sequence specific. The extension of the transcription complex into this DNA segment does suggest two possible explanations for highly diverse effects of flanking-sequence substitutions on tRNA gene transcription: either (i) proteins that are capable of binding to these upstream DNA segments are also potentially capable of stimulating or interfering with the incorporation of TFIIIB into transcription complexes or (ii) 5'-flanking sequence influences the rate of assembly of TFIIIB into stable transcription complexes.

Published

1989