Your search keyword '"Laurence H"' showing total 152 results

1. Building your own mountain: the effects, limits, and drawbacks of cold-water coral ecosystem engineering

Author

Spatial Ecology and Global Change, Geochemistry, Environmental Sciences, Climate and Environment, Van Der Kaaden, Anna Selma, Maier, Sandra R., Chen, Siluo, De Clippele, Laurence H., De Froe, Evert, Gerkema, Theo, Van De Koppel, Johan, Mienis, Furu, Mohn, Christian, Rietkerk, Max, Soetaert, Karline, Van Oevelen, Dick, Spatial Ecology and Global Change, Geochemistry, Environmental Sciences, Climate and Environment, Van Der Kaaden, Anna Selma, Maier, Sandra R., Chen, Siluo, De Clippele, Laurence H., De Froe, Evert, Gerkema, Theo, Van De Koppel, Johan, Mienis, Furu, Mohn, Christian, Rietkerk, Max, Soetaert, Karline, and Van Oevelen, Dick

Published

2024

2. Scientific concepts and methods for moving persistence assessments into the 21st century

Author

Davenport, Russell James [0000-0003-3272-4778], Hand, Laurence H. [0000-0001-8545-1633], Ortega Calvo, J. J. [0000-0003-1672-5199], Parsons, J. R. [0000-0003-1785-3627], Schaeffer, Andreas [0000-0002-4110-2631], Sweetlove, Cyril [0000-0001-7430-7732], Trapp, Stefan A.J. [0000-0001-8968-6296], Redman, Aaron D. [0000-0002-5933-7906], Davenport, Russell James, Curtis-Jackson, P., Dalkmann, Philipp, Davies, Jordan C., Fenner, Kathrin B., Hand, Laurence H., McDonough, Kathleen M., Ott, Amelie I.G., Ortega Calvo, J. J., Parsons, J. R., Schaeffer, Andreas, Sweetlove, Cyril, Trapp, Stefan A.J., Wang, Neil, Redman, Aaron D., Davenport, Russell James [0000-0003-3272-4778], Hand, Laurence H. [0000-0001-8545-1633], Ortega Calvo, J. J. [0000-0003-1672-5199], Parsons, J. R. [0000-0003-1785-3627], Schaeffer, Andreas [0000-0002-4110-2631], Sweetlove, Cyril [0000-0001-7430-7732], Trapp, Stefan A.J. [0000-0001-8968-6296], Redman, Aaron D. [0000-0002-5933-7906], Davenport, Russell James, Curtis-Jackson, P., Dalkmann, Philipp, Davies, Jordan C., Fenner, Kathrin B., Hand, Laurence H., McDonough, Kathleen M., Ott, Amelie I.G., Ortega Calvo, J. J., Parsons, J. R., Schaeffer, Andreas, Sweetlove, Cyril, Trapp, Stefan A.J., Wang, Neil, and Redman, Aaron D.

Abstract

The evaluation of a chemical substance's persistence is key to understanding its environmental fate, exposure concentration, and, ultimately, environmental risk. Traditional biodegradation test methods were developed many years ago for soluble, nonvolatile, single-constituent test substances, which do not represent the wide range of manufactured chemical substances. In addition, the Organisation for Economic Co-operation and Development (OECD) screening and simulation test methods do not fully reflect the environmental conditions into which substances are released and, therefore, estimates of chemical degradation half-lives can be very uncertain and may misrepresent real environmental processes. In this paper, we address the challenges and limitations facing current test methods and the scientific advances that are helping to both understand and provide solutions to them. Some of these advancements include the following: (1) robust methods that provide a deeper understanding of microbial composition, diversity, and abundance to ensure consistency and/or interpret variability between tests; (2) benchmarking tools and reference substances that aid in persistence evaluations through comparison against substances with well-quantified degradation profiles; (3) analytical methods that allow quantification for parent and metabolites at environmentally relevant concentrations, and inform on test substance bioavailability, biochemical pathways, rates of primary versus overall degradation, and rates of metabolite formation and decay; (4) modeling tools that predict the likelihood of microbial biotransformation, as well as biochemical pathways; and (5) modeling approaches that allow for derivation of more generally applicable biotransformation rate constants, by accounting for physical and/or chemical processes and test system design when evaluating test data. We also identify that, while such advancements could improve the certainty and accuracy of persistence assessments, th

Published

2022

3. Building your own mountain: The effects, limits, and drawbacks of cold-water coral ecosystem engineering

Author

Spatial Ecology and Global Change, Environmental Sciences, Kaaden, Anna-Selma van der, Maier, Sandra R., Chen, Siluo, Clippele, Laurence H. De, Froe, Evert de, Gerkema, Theo, Koppel, Johan van de, Mohn, Christian, Rietkerk, Max, Soetaert, Karline, Oevelen, Dick van, Spatial Ecology and Global Change, Environmental Sciences, Kaaden, Anna-Selma van der, Maier, Sandra R., Chen, Siluo, Clippele, Laurence H. De, Froe, Evert de, Gerkema, Theo, Koppel, Johan van de, Mohn, Christian, Rietkerk, Max, Soetaert, Karline, and Oevelen, Dick van

Published

2023

4. Tiger reefs: Self‐organized regular patterns in deep‐sea cold‐water coral reefs

Author

Spatial Ecology and Global Change, Geochemistry, Environmental Sciences, Climate and Environment, Kaaden, Anna‐Selma van der, Maier, Sandra R., Siteur, Koen, Clippele, Laurence H. De, Koppel, Johan van de, Purkis, Sam J., Rietkerk, Max, Soetaert, Karline, Oevelen, Dick van, Spatial Ecology and Global Change, Geochemistry, Environmental Sciences, Climate and Environment, Kaaden, Anna‐Selma van der, Maier, Sandra R., Siteur, Koen, Clippele, Laurence H. De, Koppel, Johan van de, Purkis, Sam J., Rietkerk, Max, Soetaert, Karline, and Oevelen, Dick van

Published

2023

5. On the paradox of thriving cold-water coral reefs in the food-limited deep sea

Author

Maier, Sandra R., Brooke, Sandra, De Clippele, Laurence H., de Froe, Evert, van der Kaaden, Anna Selma, Kutti, Tina, Mienis, Furu, van Oevelen, Dick, Maier, Sandra R., Brooke, Sandra, De Clippele, Laurence H., de Froe, Evert, van der Kaaden, Anna Selma, Kutti, Tina, Mienis, Furu, and van Oevelen, Dick

Abstract

The deep sea is amongst the most food-limited habitats on Earth, as only a small fraction (<4%) of the surface primary production is exported below 200 m water depth. Here, cold-water coral (CWC) reefs form oases of life: their biodiversity compares with tropical coral reefs, their biomass and metabolic activity exceed other deep-sea ecosystems by far. We critically assess the paradox of thriving CWC reefs in the food-limited deep sea, by reviewing the literature and open-access data on CWC habitats. This review shows firstly that CWCs typically occur in areas where the food supply is not constantly low, but undergoes pronounced temporal variation. High currents, downwelling and/or vertically migrating zooplankton temporally boost the export of surface organic matter to the seabed, creating ‘feast’ conditions, interspersed with ‘famine’ periods during the non-productive season. Secondly, CWCs, particularly the most common reef-builder Desmophyllum pertusum (formerly known as Lophelia pertusa), are well adapted to these fluctuations in food availability. Laboratory and in situ measurements revealed their dietary flexibility, tissue reserves, and temporal variation in growth and energy allocation. Thirdly, the high structural and functional diversity of CWC reefs increases resource retention: acting as giant filters and sustaining complex food webs with diverse recycling pathways, the reefs optimise resource gains over losses. Anthropogenic pressures, including climate change and ocean acidification, threaten this fragile equilibrium through decreased resource supply, increased energy costs, and dissolution of the calcium-carbonate reef framework. Based on this review, we suggest additional criteria to judge the health of CWC reefs and their chance to persist in the future.

Published

2023

6. Recovery and restoration potential of cold‐water corals: experience from a deep‐sea marine protected area

Author

Strong, James A., Piechaud, Nils, De Clippele, Laurence H., Bett, Brian J., Horton, Tammy, Corbera, Guillem, Huvenne, Veerle A. I., Strong, James A., Piechaud, Nils, De Clippele, Laurence H., Bett, Brian J., Horton, Tammy, Corbera, Guillem, and Huvenne, Veerle A. I.

Abstract

Cold-water corals (CWCs) are important species that provide habitat for other taxa but are sensitive to mechanical damage from bottom trawling. CWC conservation has been implemented in the form of marine protected areas (MPAs), but recovery from impact may be particularly slow in the deep-sea environment; consequently, the use of restoration techniques has been considered. To gain some insight into CWC recruitment and growth, in 2011 we deployed small seabed moorings in the Darwin Mounds MPA (~1,000 m water depth). This site hosts hundreds of CWC mounds, that had previously (until 2003) been impacted by deep-water trawling. In 2019, we carried out in situ visual surveys of these moorings and the surrounding seabed environment, then recovered two of the moorings. The mooring buoys, glass floats with plastic covers, were extensively colonized by a diverse epifauna that included the CWCs Desmophyllum pertusum and D. dianthus. The presence of coral recruits indicated that environmental conditions, and larval supply, remained favorable for the settlement and growth of CWCs within the MPA. Based on our observations, we consider four possible restoration methods, together with a “do-nothing” option, for the Darwin Mounds CWCs that have shown little, if any, natural recovery despite 16 years of protection. We conclude that seabed emplacement of high-relief artificial substrata is likely to be the most efficient and cost-efficient means of promoting enhanced recovery of the CWCs.

Published

2023

7. Recovery and restoration potential of cold-water corals: experience from a deep-sea marine protected area

Author

Natural Environment Research Council (UK), European Commission, Agencia Estatal de Investigación (España), Strong, James Asa, Piechaud, Nils, De Clippele, Laurence H., Bett, Brian J., Horton, Tammy, Corbera, Guillem, Huvenne, Veerle A.I., Natural Environment Research Council (UK), European Commission, Agencia Estatal de Investigación (España), Strong, James Asa, Piechaud, Nils, De Clippele, Laurence H., Bett, Brian J., Horton, Tammy, Corbera, Guillem, and Huvenne, Veerle A.I.

Abstract

Cold-water corals (CWCs) are important species that provide habitat for other taxa but are sensitive to mechanical damage from bottom trawling. CWC conservation has been implemented in the form of marine protected areas (MPAs), but recovery from impact may be particularly slow in the deep-sea environment; consequently, the use of restoration techniques has been considered. To gain some insight into CWC recruitment and growth, in 2011 we deployed small seabed moorings in the Darwin Mounds MPA (~1,000 m water depth). This site hosts hundreds of CWC mounds, that had previously (until 2003) been impacted by deep-water trawling. In 2019, we carried out in situ visual surveys of these moorings and the surrounding seabed environment, then recovered two of the moorings. The mooring buoys, glass floats with plastic covers, were extensively colonized by a diverse epifauna that included the CWCs Desmophyllum pertusum and D. dianthus. The presence of coral recruits indicated that environmental conditions, and larval supply, remained favorable for the settlement and growth of CWCs within the MPA. Based on our observations, we consider four possible restoration methods, together with a “do-nothing” option, for the Darwin Mounds CWCs that have shown little, if any, natural recovery despite 16 years of protection. We conclude that seabed emplacement of high-relief artificial substrata is likely to be the most efficient and cost-efficient means of promoting enhanced recovery of the CWC

Published

2023

8. Biosynthesis and mechanism of action of antitumor antibiotics

Author

Hurley, Laurence H.

Subjects

615.1

Published

1996

9. Genetic Factors Associated with Prostate Cancer Conversion from Active Surveillance to Treatment.

Author

Jiang, Yu, Jiang, Yu, Meyers, Travis J, Emeka, Adaeze A, Cooley, Lauren Folgosa, Cooper, Phillip R, Lancki, Nicola, Helenowski, Irene, Kachuri, Linda, Lin, Daniel W, Stanford, Janet L, Newcomb, Lisa F, Kolb, Suzanne, Finelli, Antonio, Fleshner, Neil E, Komisarenko, Maria, Eastham, James A, Ehdaie, Behfar, Benfante, Nicole, Logothetis, Christopher J, Gregg, Justin R, Perez, Cherie A, Garza, Sergio, Kim, Jeri, Marks, Leonard S, Delfin, Merdie, Barsa, Danielle, Vesprini, Danny, Klotz, Laurence H, Loblaw, Andrew, Mamedov, Alexandre, Goldenberg, S Larry, Higano, Celestia S, Spillane, Maria, Wu, Eugenia, Carter, H Ballentine, Pavlovich, Christian P, Mamawala, Mufaddal, Landis, Tricia, Carroll, Peter R, Chan, June M, Cooperberg, Matthew R, Cowan, Janet E, Morgan, Todd M, Siddiqui, Javed, Martin, Rabia, Klein, Eric A, Brittain, Karen, Gotwald, Paige, Barocas, Daniel A, Dallmer, Jeremiah R, Gordetsky, Jennifer B, Steele, Pam, Kundu, Shilajit D, Stockdale, Jazmine, Roobol, Monique J, Venderbos, Lionne DF, Sanda, Martin G, Arnold, Rebecca, Patil, Dattatraya, Evans, Christopher P, Dall'Era, Marc A, Vij, Anjali, Costello, Anthony J, Chow, Ken, Corcoran, Niall M, Rais-Bahrami, Soroush, Phares, Courtney, Scherr, Douglas S, Flynn, Thomas, Karnes, R Jeffrey, Koch, Michael, Dhondt, Courtney Rose, Nelson, Joel B, McBride, Dawn, Cookson, Michael S, Stratton, Kelly L, Farriester, Stephen, Hemken, Erin, Stadler, Walter M, Pera, Tuula, Banionyte, Deimante, Bianco, Fernando J, Lopez, Isabel H, Loeb, Stacy, Taneja, Samir S, Byrne, Nataliya, Amling, Christopher L, Martinez, Ann, Boileau, Luc, Gaylis, Franklin D, Petkewicz, Jacqueline, Kirwen, Nicholas, Helfand, Brian T, Xu, Jianfeng, Scholtens, Denise M, Catalona, William J, Witte, John S, Jiang, Yu, Jiang, Yu, Meyers, Travis J, Emeka, Adaeze A, Cooley, Lauren Folgosa, Cooper, Phillip R, Lancki, Nicola, Helenowski, Irene, Kachuri, Linda, Lin, Daniel W, Stanford, Janet L, Newcomb, Lisa F, Kolb, Suzanne, Finelli, Antonio, Fleshner, Neil E, Komisarenko, Maria, Eastham, James A, Ehdaie, Behfar, Benfante, Nicole, Logothetis, Christopher J, Gregg, Justin R, Perez, Cherie A, Garza, Sergio, Kim, Jeri, Marks, Leonard S, Delfin, Merdie, Barsa, Danielle, Vesprini, Danny, Klotz, Laurence H, Loblaw, Andrew, Mamedov, Alexandre, Goldenberg, S Larry, Higano, Celestia S, Spillane, Maria, Wu, Eugenia, Carter, H Ballentine, Pavlovich, Christian P, Mamawala, Mufaddal, Landis, Tricia, Carroll, Peter R, Chan, June M, Cooperberg, Matthew R, Cowan, Janet E, Morgan, Todd M, Siddiqui, Javed, Martin, Rabia, Klein, Eric A, Brittain, Karen, Gotwald, Paige, Barocas, Daniel A, Dallmer, Jeremiah R, Gordetsky, Jennifer B, Steele, Pam, Kundu, Shilajit D, Stockdale, Jazmine, Roobol, Monique J, Venderbos, Lionne DF, Sanda, Martin G, Arnold, Rebecca, Patil, Dattatraya, Evans, Christopher P, Dall'Era, Marc A, Vij, Anjali, Costello, Anthony J, Chow, Ken, Corcoran, Niall M, Rais-Bahrami, Soroush, Phares, Courtney, Scherr, Douglas S, Flynn, Thomas, Karnes, R Jeffrey, Koch, Michael, Dhondt, Courtney Rose, Nelson, Joel B, McBride, Dawn, Cookson, Michael S, Stratton, Kelly L, Farriester, Stephen, Hemken, Erin, Stadler, Walter M, Pera, Tuula, Banionyte, Deimante, Bianco, Fernando J, Lopez, Isabel H, Loeb, Stacy, Taneja, Samir S, Byrne, Nataliya, Amling, Christopher L, Martinez, Ann, Boileau, Luc, Gaylis, Franklin D, Petkewicz, Jacqueline, Kirwen, Nicholas, Helfand, Brian T, Xu, Jianfeng, Scholtens, Denise M, Catalona, William J, and Witte, John S

Abstract

Men diagnosed with low-risk prostate cancer (PC) are increasingly electing active surveillance (AS) as their initial management strategy. While this may reduce the side effects of treatment for prostate cancer, many men on AS eventually convert to active treatment. PC is one of the most heritable cancers, and genetic factors that predispose to aggressive tumors may help distinguish men who are more likely to discontinue AS. To investigate this, we undertook a multi-institutional genome-wide association study (GWAS) of 5,222 PC patients and 1,139 other patients from replication cohorts, all of whom initially elected AS and were followed over time for the potential outcome of conversion from AS to active treatment. In the GWAS we detected 18 variants associated with conversion, 15 of which were not previously associated with PC risk. With a transcriptome-wide association study (TWAS), we found two genes associated with conversion (MAST3, p = 6.9×10-7 and GAB2, p = 2.0×10-6). Moreover, increasing values of a previously validated 269-variant genetic risk score (GRS) for PC was positively associated with conversion (e.g., comparing the highest to the two middle deciles gave a hazard ratio [HR] = 1.13; 95% Confidence Interval [CI]= 0.94-1.36); whereas, decreasing values of a 36-variant GRS for prostate-specific antigen (PSA) levels were positively associated with conversion (e.g., comparing the lowest to the two middle deciles gave a HR = 1.25; 95% CI, 1.04-1.50). These results suggest that germline genetics may help inform and individualize the decision of AS-or the intensity of monitoring on AS-versus treatment for the initial management of patients with low-risk PC.

Published

2022

10. Caracterización de los tipos de respuesta de parpadeo en un procedimiento de condicionamiento discriminativo en humanos

Author

Tapia, Laurence H., Becerra Céspedes, Sebastián Agustín, Pinto Pinto, Jorge Andrés, Tapia, Laurence H., Becerra Céspedes, Sebastián Agustín, and Pinto Pinto, Jorge Andrés

Abstract

We report the results of a human eyeblink conditioning procedure aimed at characterizing different types of responses. To do this, eight participants received an auditory conditioned stimulus paired with an unconditioned stimulus -air puff in the eye-and a vibro-tactile stimulus non reinforced. We demonstrated the existence of four responses. In the first 100 milliseconds (ms) since the initiation of conditioned a small amplitude response, called alpha, appears, which is followed by intermediate amplitude responses, called voluntary(200-300 ms) and conditioned(300-400 ms). Finally, the largest-amplitude responses occur about 200 ms after unconditioned stimulus onset. Both voluntary and conditioned responses are more frequent in the presence of stimulus A that B. We discuss the relevance of identifying and distinguishing these types of responses in any classical conditioning routine., Se reportaron los resultados de un procedimiento de condicionamiento palpebral en humanos destinado a caracterizar distintos tipos de respuestas. Para ello, ocho participantes recibieron un estímulo condicionado auditivo emparejado con un estímulo incondicionado, soplo de aire en el ojo, mientras que un estímulo condicionado vibro-táctil no fue reforzado. Se demostró la existencia de cuatro repuestas. En los primeros 100 milisegundos (ms) desde la iniciación de los estímulos condicionados ocurren respuestas de pequeña amplitud, denominadas alfa, a las cuales le siguen otras respuestas de amplitud intermedia, denominadas voluntarias (200-300 ms) y condicionadas (300-400 ms). Finalmente, las respuestas incondicionadas ocurren en los 200 ms que siguen el inicio del estímulo incondicionado y son de gran amplitud. Tanto las respuestas voluntarias como condicionadas son más frecuentes en presencia del estímulo A que B. Discutimos la relevancia de identificar y distinguir estos tipos de respuestas en cualquier rutina de condicionamiento clásico.

Published

2022

11. Serine Protease HTRA1 as a Novel Target Antigen in Primary Membranous Nephropathy

Author

Al-Rabadi, Laith Farah, Caza, Tiffany, Trivin-Avillach, Claire, Rodan, Aylin R., Andeen, Nicole, Hayashi, Norifumi, Williams, Brandi, Revelo, Monica P., Clayton, Fred, Abraham, Jo, Lin, Edwin, Liou, Willisa, Zou, Chang-Jiang, Ramkumar, Nirupama, Cummins, Tim, Wilkey, Daniel W., Kawalit, Issa, Herzog, Christian, Storey, Aaron, Edmondson, Rick, Sjöberg, Ronald, Yang, Tianxin, Chien, Jeremy, Merchant, Michael, Arthur, John, Klein, Jon, Larsen, Chris, Beck, Laurence H., Al-Rabadi, Laith Farah, Caza, Tiffany, Trivin-Avillach, Claire, Rodan, Aylin R., Andeen, Nicole, Hayashi, Norifumi, Williams, Brandi, Revelo, Monica P., Clayton, Fred, Abraham, Jo, Lin, Edwin, Liou, Willisa, Zou, Chang-Jiang, Ramkumar, Nirupama, Cummins, Tim, Wilkey, Daniel W., Kawalit, Issa, Herzog, Christian, Storey, Aaron, Edmondson, Rick, Sjöberg, Ronald, Yang, Tianxin, Chien, Jeremy, Merchant, Michael, Arthur, John, Klein, Jon, Larsen, Chris, and Beck, Laurence H.

Abstract

Background Identification of target antigens PLA2R, THSD7A, NELL1, or Semaphorin-3B can explain the majority of cases of primary membranous nephropathy (MN). However, target antigens remain unidentified in 15%-20% of patients. Methods A multipronged approach, using traditional and modern technologies, converged on a novel target antigen, and capitalized on the temporal variation in autoantibody titer for biomarker discovery. Immunoblotting of human glomerular proteins followed by differential immunoprecipitation and mass spectrometric analysis was complemented by laser-capture microdissection followed by mass spectrometry, elution of immune complexes from renal biopsy specimen tissue, and autoimmune profiling on a protein fragment microarray. Results These approaches identified serine protease HTRA1 as a novel podocyte antigen in a subset of patients with primary MN. Sera from two patients reacted by immunoblotting with a 51-kD protein within glomerular extract and with recombinant human HTRA1, under reducing and nonreducing conditions. Longitudinal serum samples from these patients seemed to correlate with clinical disease activity. As in PLA2R- and THSD7A- associated MN, anti-HTRA1 antibodies were predominantly IgG4, suggesting a primary etiology. Analysis of sera collected during active disease versus remission on protein fragment microarrays detected significantly higher titers of anti-HTRA1 antibody in active disease. HTRA1 was specifically detected within immune deposits of HTRA1-associated MN in 14 patients identified among three cohorts. Screening of 118 "quadruple-negative" (PLA2R-, THSD7A-, NELL1-, EXT2-negative) patients in a large repository of MN biopsy specimens revealed a prevalence of 4.2%. Conclusions Conventional and more modern techniques converged to identify serine protease HTRA1 as a target antigen in MN., QC 20220224

Published

2021

12. Altered glycosylation of IgG4 promotes lectin complement pathway activation in anti-PLA2R1-associated membranous nephropathy

Author

Haddad, George, Lorenzen, Johan M; https://orcid.org/0000-0002-9132-948X, Ma, Hong, de Haan, Noortje, Seeger, Harald; https://orcid.org/0000-0003-1552-7983, Zaghrini, Christelle, Brandt, Simone; https://orcid.org/0000-0002-8558-6674, Kölling, Malte; https://orcid.org/0000-0002-6396-2069, Wegmann, Urs, Kiss, Bence, Pál, Gábor, Gál, Péter, Wüthrich, Rudolf P; https://orcid.org/0000-0002-5425-6453, Wuhrer, Manfred, Beck, Laurence H, Salant, David J, Lambeau, Gérard, Kistler, Andreas D, Haddad, George, Lorenzen, Johan M; https://orcid.org/0000-0002-9132-948X, Ma, Hong, de Haan, Noortje, Seeger, Harald; https://orcid.org/0000-0003-1552-7983, Zaghrini, Christelle, Brandt, Simone; https://orcid.org/0000-0002-8558-6674, Kölling, Malte; https://orcid.org/0000-0002-6396-2069, Wegmann, Urs, Kiss, Bence, Pál, Gábor, Gál, Péter, Wüthrich, Rudolf P; https://orcid.org/0000-0002-5425-6453, Wuhrer, Manfred, Beck, Laurence H, Salant, David J, Lambeau, Gérard, and Kistler, Andreas D

Abstract

Primary membranous nephropathy (pMN) is a leading cause of nephrotic syndrome in adults. In most cases, this autoimmune kidney disease is associated with autoantibodies against the M-type phospholipase A2 receptor (PLA2R1) expressed on kidney podocytes, but the mechanisms leading to glomerular damage remain elusive. Here, we developed a cell culture model using human podocytes and found that anti-PLA2R1-positive pMN patient sera or isolated IgG4, but not IgG4-depleted sera, induced proteolysis of the 2 essential podocyte proteins synaptopodin and NEPH1 in the presence of complement, resulting in perturbations of the podocyte cytoskeleton. Specific blockade of the lectin pathway prevented degradation of synaptopodin and NEPH1. Anti-PLA2R1 IgG4 directly bound mannose-binding lectin in a glycosylation-dependent manner. In a cohort of pMN patients, we identified increased levels of galactose-deficient IgG4, which correlated with anti-PLA2R1 titers and podocyte damage induced by patient sera. Assembly of the terminal C5b-9 complement complex and activation of the complement receptors C3aR1 or C5aR1 were required to induce proteolysis of synaptopodin and NEPH1 by 2 distinct proteolytic pathways mediated by cysteine and aspartic proteinases, respectively. Together, these results demonstrated a mechanism by which aberrantly glycosylated IgG4 activated the lectin pathway and induced podocyte injury in primary membranous nephropathy. Keywords: Chronic kidney disease; Complement; Glycobiology; Immunology; Nephrology.

Published

2021

13. Prostate cancer mortality and metastasis under different biopsy frequencies in North American active surveillance cohorts

Author

Lange, Jane M., Laviana, Aaron A., Penson, David F., Lin, Daniel W., Bill-Axelson, Anna, Carlsson, Sigrid, V, Newcomb, Lisa F., Trock, Bruce J., Carter, H. Ballentine, Carroll, Peter R., Cooperberg, Mathew R., Cowan, Janet E., Klotz, Laurence H., Etzioni, Ruth B., Lange, Jane M., Laviana, Aaron A., Penson, David F., Lin, Daniel W., Bill-Axelson, Anna, Carlsson, Sigrid, V, Newcomb, Lisa F., Trock, Bruce J., Carter, H. Ballentine, Carroll, Peter R., Cooperberg, Mathew R., Cowan, Janet E., Klotz, Laurence H., and Etzioni, Ruth B.

Abstract

Background Active surveillance (AS) is an accepted means of managing low-risk prostate cancer. Because of the rarity of downstream events, data from existing AS cohorts cannot yet address how differences in surveillance intensity affect metastasis and mortality. This study projected the comparative benefits of different AS schedules in men diagnosed with prostate cancer who had Gleason score (GS) <= 6 disease and risk profiles similar to those in North American AS cohorts. Methods Times of GS upgrading were simulated based on AS data from the University of Toronto, Johns Hopkins University, the University of California at San Francisco, and the Canary Pass Active Surveillance Cohort. Times to metastasis and prostate cancer death, informed by models from the Scandinavian Prostate Cancer Group 4 trial, were projected under biopsy surveillance schedules ranging from watchful waiting to annual biopsies. Outcomes included the risk of metastasis, the risk of death, remaining life-years (LYs), and quality-adjusted LYs. Results Compared with watchful waiting, AS biopsies reduced the risk of prostate cancer metastasis and prostate cancer death at 20 years by 1.4% to 3.3% and 1.0% to 2.4%, respectively; and 5-year biopsies reduced the risk of metastasis and prostate cancer death by 1.0% to 2.4% and 0.6% to 1.6%, respectively. There was little difference between annual and 5-year biopsy schedules in terms of LYs (range of differences, 0.04-0.16 LYs) and quality-adjusted LYs (range of differences, -0.02 to 0.09 quality-adjusted LYs). Conclusions Among men diagnosed with GS <= 6 prostate cancer, obtaining a biopsy every 3 or 4 years appears to be an acceptable alternative to more frequent biopsies. Reducing surveillance intensity for those who have a low risk of progression reduces the number of biopsies while preserving the benefit of more frequent schedules.

Published

2020

14. Prostate cancer mortality and metastasis under different biopsy frequencies in North American active surveillance cohorts.

Author

Lange, Jane M, Lange, Jane M, Laviana, Aaron A, Penson, David F, Lin, Daniel W, Bill-Axelson, Anna, Carlsson, Sigrid V, Newcomb, Lisa F, Trock, Bruce J, Carter, H Ballentine, Carroll, Peter R, Cooperberg, Mathew R, Cowan, Janet E, Klotz, Laurence H, Etzioni, Ruth B, Lange, Jane M, Lange, Jane M, Laviana, Aaron A, Penson, David F, Lin, Daniel W, Bill-Axelson, Anna, Carlsson, Sigrid V, Newcomb, Lisa F, Trock, Bruce J, Carter, H Ballentine, Carroll, Peter R, Cooperberg, Mathew R, Cowan, Janet E, Klotz, Laurence H, and Etzioni, Ruth B

Abstract

BackgroundActive surveillance (AS) is an accepted means of managing low-risk prostate cancer. Because of the rarity of downstream events, data from existing AS cohorts cannot yet address how differences in surveillance intensity affect metastasis and mortality. This study projected the comparative benefits of different AS schedules in men diagnosed with prostate cancer who had Gleason score (GS) ≤6 disease and risk profiles similar to those in North American AS cohorts.MethodsTimes of GS upgrading were simulated based on AS data from the University of Toronto, Johns Hopkins University, the University of California at San Francisco, and the Canary Pass Active Surveillance Cohort. Times to metastasis and prostate cancer death, informed by models from the Scandinavian Prostate Cancer Group 4 trial, were projected under biopsy surveillance schedules ranging from watchful waiting to annual biopsies. Outcomes included the risk of metastasis, the risk of death, remaining life-years (LYs), and quality-adjusted LYs.ResultsCompared with watchful waiting, AS biopsies reduced the risk of prostate cancer metastasis and prostate cancer death at 20 years by 1.4% to 3.3% and 1.0% to 2.4%, respectively; and 5-year biopsies reduced the risk of metastasis and prostate cancer death by 1.0% to 2.4% and 0.6% to 1.6%, respectively. There was little difference between annual and 5-year biopsy schedules in terms of LYs (range of differences, 0.04-0.16 LYs) and quality-adjusted LYs (range of differences, -0.02 to 0.09 quality-adjusted LYs).ConclusionsAmong men diagnosed with GS ≤6 prostate cancer, obtaining a biopsy every 3 or 4 years appears to be an acceptable alternative to more frequent biopsies. Reducing surveillance intensity for those who have a low risk of progression reduces the number of biopsies while preserving the benefit of more frequent schedules.

Published

2020

15. Systematic evaluation of velocity-selective arterial spin labeling settings for placental perfusion measurement

Author

Researchgr. Beeldg. Moleculaire Interv., Brain, Circulatory Health, Cancer, Harteveld, Anita A, Hutter, Jana, Franklin, Suzanne L, Jackson, Laurence H, Rutherford, Mary, Hajnal, Joseph V, van Osch, Matthias J P, Bos, Clemens, De Vita, Enrico, Researchgr. Beeldg. Moleculaire Interv., Brain, Circulatory Health, Cancer, Harteveld, Anita A, Hutter, Jana, Franklin, Suzanne L, Jackson, Laurence H, Rutherford, Mary, Hajnal, Joseph V, van Osch, Matthias J P, Bos, Clemens, and De Vita, Enrico

Published

2020

16. Perfusion and apparent oxygenation in the human placenta (PERFOX)

Author

Brain, Circulatory Health, Researchgr. Beeldg. Moleculaire Interv., Cancer, Hutter, Jana, Harteveld, Anita A, Jackson, Laurence H, Franklin, Suzanne, Bos, Clemens, van Osch, Matthias J P, O'Muircheartaigh, Jonathan, Ho, Alison, Chappell, Lucy, Hajnal, Joseph V, Rutherford, Mary, De Vita, Enrico, Brain, Circulatory Health, Researchgr. Beeldg. Moleculaire Interv., Cancer, Hutter, Jana, Harteveld, Anita A, Jackson, Laurence H, Franklin, Suzanne, Bos, Clemens, van Osch, Matthias J P, O'Muircheartaigh, Jonathan, Ho, Alison, Chappell, Lucy, Hajnal, Joseph V, Rutherford, Mary, and De Vita, Enrico

Published

2020

17. MDC1 Interacts with TOPBP1 to Maintain Chromosomal Stability during Mitosis

Author

Leimbacher, Pia-Amata, Jones, Samuel E, Shorrocks, Ann-Marie K, de Marco Zompit, Mara, Day, Matthew, Blaauwendraad, Jordy, Bundschuh, Diana, Bonham, Sarah, Fischer, Roman, Fink, Daniel, Kessler, Benedikt M, Oliver, Antony W, Pearl, Laurence H, Blackford, Andrew N, Stucki, Manuel, Leimbacher, Pia-Amata, Jones, Samuel E, Shorrocks, Ann-Marie K, de Marco Zompit, Mara, Day, Matthew, Blaauwendraad, Jordy, Bundschuh, Diana, Bonham, Sarah, Fischer, Roman, Fink, Daniel, Kessler, Benedikt M, Oliver, Antony W, Pearl, Laurence H, Blackford, Andrew N, and Stucki, Manuel

Abstract

In mitosis, cells inactivate DNA double-strand break (DSB) repair pathways to preserve genome stability. However, some early signaling events still occur, such as recruitment of the scaffold protein MDC1 to phosphorylated histone H2AX at DSBs. Yet, it remains unclear whether these events are important for maintaining genome stability during mitosis. Here, we identify a highly conserved protein-interaction surface in MDC1 that is phosphorylated by CK2 and recognized by the DNA-damage response mediator protein TOPBP1. Disruption of MDC1-TOPBP1 binding causes a specific loss of TOPBP1 recruitment to DSBs in mitotic but not interphase cells, accompanied by mitotic radiosensitivity, increased micronuclei, and chromosomal instability. Mechanistically, we find that TOPBP1 forms filamentous structures capable of bridging MDC1 foci in mitosis, indicating that MDC1-TOPBP1 complexes tether DSBs until repair is reactivated in the following G1 phase. Thus, we reveal an important, hitherto-unnoticed cooperation between MDC1 and TOPBP1 in maintaining genome stability during cell division.

Published

2019

18. Self-supervised Recurrent Neural Network for 4D Abdominal and In-utero MR Imaging

Author

Zhang, Tong, Jackson, Laurence H., Uus, Alena, Clough, James R., Story, Lisa, Rutherford, Mary A., Hajnal, Joseph V., Deprez, Maria, Zhang, Tong, Jackson, Laurence H., Uus, Alena, Clough, James R., Story, Lisa, Rutherford, Mary A., Hajnal, Joseph V., and Deprez, Maria

Abstract

Accurately estimating and correcting the motion artifacts are crucial for 3D image reconstruction of the abdominal and in-utero magnetic resonance imaging (MRI). The state-of-art methods are based on slice-to-volume registration (SVR) where multiple 2D image stacks are acquired in three orthogonal orientations. In this work, we present a novel reconstruction pipeline that only needs one orientation of 2D MRI scans and can reconstruct the full high-resolution image without masking or registration steps. The framework consists of two main stages: the respiratory motion estimation using a self-supervised recurrent neural network, which learns the respiratory signals that are naturally embedded in the asymmetry relationship of the neighborhood slices and cluster them according to a respiratory state. Then, we train a 3D deconvolutional network for super-resolution (SR) reconstruction of the sparsely selected 2D images using integrated reconstruction and total variation loss. We evaluate the classification accuracy on 5 simulated images and compare our results with the SVR method in adult abdominal and in-utero MRI scans. The results show that the proposed pipeline can accurately estimate the respiratory state and reconstruct 4D SR volumes with better or similar performance to the 3D SVR pipeline with less than 20\% sparsely selected slices. The method has great potential to transform the 4D abdominal and in-utero MRI in clinical practice., Comment: Accepted by MICCAI 2019 workshop on Machine Learning for Medical Image Reconstruction

Published

2019

19. Analyse de processus d'implantation des ruelles vertes à Montréal et recommandations pour les porteurs de projets

Author

Lauzon, Sophie-Laurence H., Villeneuve, Carole, Lauzon, Sophie-Laurence H., and Villeneuve, Carole

Abstract

Les ruelles montréalaises, des espaces urbains sous-utilisés et aux prises avec différentes problématiques, notamment de sécurité et d'apparence, sont pourtant des espaces publics au potentiel notable et requérant une attention particulière. Les efforts de revitalisation menés dans les ruelles proposent un changement de paradigme dans la façon d'aborder cet espace urbain. Offrant une seconde vie aux ruelles, les projets de ruelle verte se présentent justement comme des efforts de verdissement participatifs qui s’inscrivent dans un développement urbain durable. L'implantation de ce type de projet n'est pourtant pas sans défi, et plusieurs améliorations sont possibles. L'objectif général de cet essai est donc d'analyser des processus d'implantation des ruelles vertes à Montréal afin d'émettre des recommandations aux porteurs de projets. L'analyse permet de mettre en lumière les potentiels, les contraintes, les points forts et les points faibles des programmes et projets de ruelle verte. En appui à une analyse générale sur les processus d'implantation des ruelles vertes à Montréal, deux études de cas s'intéressent spécifiquement aux arrondissements Le Plateau-Mont-Royal et le Sud-Ouest. Celles-ci s'appuient sur des critères qui couvrent les différentes phases des processus et les dimensions du développement durable. À la suite de cette analyse, il est possible de constater que, bien que certaines contraintes imposent des limites physiques, de mobilisation citoyenne et autres, il n'en reste pas moins que les projets de ruelle verte présentent un potentiel considérable en matière environnementale, par le retour de service écologique, et sociale, notamment par la création de liens communautaires. Alors que les projets de la métropole rayonnent et que les apports de la démarche participative placent les comités citoyens au cœur de la prise de décision, des manques importants pour assurer le succès et la pérennité des projets persistent, notamment le manque de mécanismes de

Published

2019

20. Comparative Analysis of Biopsy Upgrading in Four Prostate Cancer Active Surveillance Cohorts.

Author

Inoue, Lurdes YT, Inoue, Lurdes YT, Lin, Daniel W, Newcomb, Lisa F, Leonardson, Amy S, Ankerst, Donna, Gulati, Roman, Carter, H Ballentine, Trock, Bruce J, Carroll, Peter R, Cooperberg, Matthew R, Cowan, Janet E, Klotz, Laurence H, Mamedov, Alexandre, Penson, David F, Etzioni, Ruth, Inoue, Lurdes YT, Inoue, Lurdes YT, Lin, Daniel W, Newcomb, Lisa F, Leonardson, Amy S, Ankerst, Donna, Gulati, Roman, Carter, H Ballentine, Trock, Bruce J, Carroll, Peter R, Cooperberg, Matthew R, Cowan, Janet E, Klotz, Laurence H, Mamedov, Alexandre, Penson, David F, and Etzioni, Ruth

Abstract

BackgroundActive surveillance (AS) is increasingly accepted for managing low-risk prostate cancer, yet there is no consensus about implementation. This lack of consensus is due in part to uncertainty about risks for disease progression, which have not been systematically compared or integrated across AS studies with variable surveillance protocols and dropout to active treatment.ObjectiveTo compare risks for upgrading from a Gleason score (GS) of 6 or less to 7 or more across AS studies after accounting for differences in surveillance intervals and competing treatments and to evaluate tradeoffs of more versus less frequent biopsies.DesignJoint statistical model of longitudinal prostate-specific antigen (PSA) levels and risks for biopsy upgrading.SettingJohns Hopkins University (JHU); Canary Prostate Active Surveillance Study (PASS); University of California, San Francisco (UCSF); and University of Toronto (UT) AS studies.Patients2576 men aged 40 to 80 years with a GS between 2 and 6 and clinical stage T1 or T2 prostate cancer enrolled between 1995 and 2014.MeasurementsPSA levels and biopsy GSs.ResultsAfter variable surveillance intervals and competing treatments were accounted for, estimated risks for biopsy upgrading were similar in the PASS and UT studies but higher in UCSF and lower in JHU studies. All cohorts had a delay of 3 to 5 months in detecting upgrading with biennial biopsies starting after a first confirmatory biopsy versus annual biopsies.LimitationThe model does not account for possible misclassification of biopsy GS.ConclusionMen in different AS studies have different risks for biopsy upgrading after variable surveillance protocols and competing treatments are accounted for. Despite these differences, the consequences of more versus less frequent biopsies seem to be similar across cohorts. Biennial biopsies seem to be an acceptable alternative to annual biopsies.Primary funding sourceNational Cancer Institute.

Published

2018

21. Advances on the Structure of the R2TP/Prefoldin-like Complex

Author

Djouder, Nabil, Munoz-Hernandez, Hugo, Pal, Mohinder, Rodriquez, Carlos F., Prodromou, Chrisostomos, Pearl, Laurence H., Llorca, Oscar, Djouder, Nabil, Munoz-Hernandez, Hugo, Pal, Mohinder, Rodriquez, Carlos F., Prodromou, Chrisostomos, Pearl, Laurence H., and Llorca, Oscar

Abstract

Cellular stability, assembly and activation of a growing list of macromolecular complexes require the action of HSP90 working in concert with the R2TP/Prefoldin-like (R2TP/PFDL) co-chaperone. RNA polymerase II, snoRNPs and complexes of PI3-kinase-like kinases, a family that includes the ATM, ATR, DNA-PKcs, TRAPP, SMG1 and mTOR proteins, are among the clients of the HSP90-R2TP system. Evidence links the R2TP/PFDL pathway with cancer, most likely because of the essential role in pathways commonly deregulated in cancer. R2TP forms the core of the co-cochaperone and orchestrates the recruitment of HSP90 and clients, whereas prefoldin and additional prefoldin-like proteins, including URI, associate with R2TP, but their function is still unclear. The mechanism by which R2TP/PFLD facilitates assembly and activation of such a variety of macromolecular complexes is poorly understood. Recent efforts in the structural characterization of R2TP have started to provide some mechanistic insights. We summarize recent structural findings, particularly how cryo-electron microscopy (cryo-EM) is contributing to our understanding of the architecture of the R2TP core complex. Structural differences discovered between yeast and human R2TP reveal unanticipated complexities of the metazoan R2TP complex, and opens new and interesting questions about how R2TP/PFLD works.

Published

2018

22. Complex congenital heart disease associated with disordered myocardial architecture in a midtrimester Human Fetus

Author

Ministerio de Economía y Competitividad (España), European Commission, Fundació La Marató de TV3, British Heart Foundation, Garcia-Canadilla, Patricia, Dejea, Hector, Bonnin, Anne, Balicevic, Vedrana, Loncaric, Sven, Zhang, Chong, Butakoff, Constantine, Aguado-Sierra, Jazmin, Vazquez, Mariano, Jackson, Laurence H., Stuckey, Daniel J., Rau, Cristoph, Stampanoni, Marco, Bijnens, Bart, Cook, Andrew C., Ministerio de Economía y Competitividad (España), European Commission, Fundació La Marató de TV3, British Heart Foundation, Garcia-Canadilla, Patricia, Dejea, Hector, Bonnin, Anne, Balicevic, Vedrana, Loncaric, Sven, Zhang, Chong, Butakoff, Constantine, Aguado-Sierra, Jazmin, Vazquez, Mariano, Jackson, Laurence H., Stuckey, Daniel J., Rau, Cristoph, Stampanoni, Marco, Bijnens, Bart, and Cook, Andrew C.

Abstract

[Background]: In the era of increasingly successful corrective interventions in patients with congenital heart disease (CHD), global and regional myocardial remodeling are emerging as important sources of long-term morbidity/mortality. Changes in organization of the myocardium in CHD, and in its mechanical properties, conduction, and blood supply, result in altered myocardial function both before and after surgery. To gain a better understanding and develop appropriate and individualized treatment strategies, the microscopic organization of cardiomyocytes, and their integration at a macroscopic level, needs to be completely understood. The aim of this study is to describe, for the first time, in 3 dimensions and nondestructively the detailed remodeling of cardiac microstructure present in a human fetal heart with complex CHD. [Methods and results]: Synchrotron X-ray phase-contrast imaging was used to image an archival midgestation formalin-fixed fetal heart with right isomerism and complex CHD and compare with a control fetal heart. Analysis of myocyte aggregates, at detail not accessible with other techniques, was performed. Macroanatomic and conduction system changes specific to the disease were clearly observable, together with disordered myocyte organization in the morphologically right ventricle myocardium. Electrical activation simulations suggested altered synchronicity of the morphologically right ventricle. [Conclusions]: We have shown the potential of X-ray phase-contrast imaging for studying cardiac microstructure in the developing human fetal heart at high resolution providing novel insight while preserving valuable archival material for future study. This is the first study to show myocardial alterations occur in complex CHD as early as midgestation.

Published

2018

23. Antibiotic resistance among Helicobacter pylori clinical isolates in Lima, Peru

Author

Boehnke,Kevin F, Valdivieso,Manuel, Bussalleu,Alejandro, Sexton,Rachael, Thompson,Kathryn C, Osorio,Soledad, Novoa Reyes,Italo, Crowley,John J., Baker,Laurence H., Xi,Chuanwu, Boehnke,Kevin F, Valdivieso,Manuel, Bussalleu,Alejandro, Sexton,Rachael, Thompson,Kathryn C, Osorio,Soledad, Novoa Reyes,Italo, Crowley,John J., Baker,Laurence H., and Xi,Chuanwu

Abstract

Kevin F Boehnke,1 Manuel Valdivieso,2 Alejandro Bussalleu,3 Rachael Sexton,4 Kathryn C Thompson,1 Soledad Osorio,5 Italo Novoa Reyes,3 John J Crowley,4 Laurence H Baker,2 Chuanwu Xi1 1Department of Environmental Health Sciences, School of Public Health, 2Division of Hematology Oncology, Department of Internal Medicine, University of Michigan, Ann Arbor, MI, USA; 3Departamento Académico de Clínicas Médicas, Facultad de Medicina Alberto Hurtado, Universidad Peruana Cayetano Heredia, Lima, Perú; 4Cancer Research and Biostatistics, Seattle, WA, USA; 5Dirección General de Salud Ambiental, Ministerio de Salud del Perú, Lima, Perú Objectives: Gastric carcinoma is the most common cancer and cause of cancer mortality in Peru. Helicobacter pylori, a bacterium that colonizes the human stomach, is a Group 1 carcinogen due to its causal relationship to gastric carcinoma. While eradication of H. pylori can help prevent gastric cancer, characterizing regional antibiotic resistance patterns is necessary to determine targeted treatment for each region. Thus, we examined primary antibiotic resistance in clinical isolates of H. pylori in Lima, Peru.Materials and methods: H. pylori strains were isolated from gastric biopsies of patients with histologically proven H. pylori infection. Primary antibiotic resistance among isolates was examined using E-test strips. Isolates were examined for the presence of the cagA pathogenicity island and the vacA m1/m2 alleles via polymerase chain reaction.Results: Seventy-six isolates were recovered from gastric biopsies. Clinical isolates showed evidence of antibiotic resistance to 1 (27.6%, n=21/76), 2 (28.9%, n=22/76), or ≥3 antibiotics (40.8%). Of 76 isolates, eight (10.5%) were resistant to amoxicillin and clarithromycin, which are part of the standard triple therapy for H. pylori infection. No trends were seen between the presence of cagA, vacA m1, or vacA m2 and

Published

2017

24. The structure of the R2TP complex defines a platform for recruiting diverse client proteins to the HSP90 molecular chaperone system

Author

Ministerio de Economía y Competitividad (España), Consejo Superior de Investigaciones Científicas (España), Rivera-Calzada, Angel, Pal, Mohinder, Luque-Ortega, Juan Román, Gil-Cartón, David, Degliesposti, Gianluca, Skehel, J. Mark, Prodromou, Chrisostomos, Pearl, Laurence H., Llorca, Óscar, Ministerio de Economía y Competitividad (España), Consejo Superior de Investigaciones Científicas (España), Rivera-Calzada, Angel, Pal, Mohinder, Luque-Ortega, Juan Román, Gil-Cartón, David, Degliesposti, Gianluca, Skehel, J. Mark, Prodromou, Chrisostomos, Pearl, Laurence H., and Llorca, Óscar

Abstract

The R2TP complex, comprising the Rvb1p-Rvb2p AAA-ATPases, Tah1p, and Pih1p in yeast, is a specialized Hsp90 co-chaperone required for the assembly and maturation of multi-subunit complexes. These include the small nucleolar ribonucleoproteins, RNA polymerase II, and complexes containing phosphatidylinositol-3-kinase-like kinases. The structure and stoichiometry of yeast R2TP and how it couples to Hsp90 are currently unknown. Here, we determine the 3D organization of yeast R2TP using sedimentation velocity analysis and cryo-electron microscopy. The 359-kDa complex comprises one Rvb1p/Rvb2p hetero-hexamer with domains II (DIIs) forming an open basket that accommodates a single copy of Tah1p-Pih1p. Tah1p-Pih1p binding to multiple DII domains regulates Rvb1p/Rvb2p ATPase activity. Using domain dissection and cross-linking mass spectrometry, we identified a unique region of Pih1p that is essential for interaction with Rvb1p/Rvb2p. These data provide a structural basis for understanding how R2TP couples an Hsp90 dimer to a diverse set of client proteins and complexes.

Published

2017

25. SWOG S0701 phase III randomized trial of three antibiotic regimens to eradicate helicobacter pylori: efficacy and failure at one year

Author

Baker, Laurence H, Baker, Laurence H, Crowley, John J, Valdivieso, Manuel, Dominguez, Ricardo L, Bravo, Luis E, Pena, Rodolfo, Meza-Montenegro, Maria M, Correa, Pelayo, Chey, William D, Morgan, Douglas R, Meyskens, Frank L, Goodman, Gary E, Baker, Laurence H, Baker, Laurence H, Crowley, John J, Valdivieso, Manuel, Dominguez, Ricardo L, Bravo, Luis E, Pena, Rodolfo, Meza-Montenegro, Maria M, Correa, Pelayo, Chey, William D, Morgan, Douglas R, Meyskens, Frank L, and Goodman, Gary E

Published

2012

26. The Huguenots, the Protestant Interest, and the War of the Spanish Succession, 1702-1714

Author

Boles, Laurence H., Boles, Laurence H., Boles, Laurence H., and Boles, Laurence H.

Abstract

By 1700, the Protestants of Europe, above all the Calvinists (Reformed), felt threatened anew by Roman Catholicism. Activists, especially Huguenot émigrés, pleaded to friendly rulers to restore Protestantism in France and to protect it in the Holy Roman Empire as aims in their wars against Louis XIV. This activism peaked during the War of the Spanish Succession, 1702-1714, but to no avail. The peace of 1713-1715 brought only token gains for the continental Protestant interest; both the Allied and the Bourbon powers were absorbed in such secular concerns as state sovereignty, dynasticism, collective security, and trade. The activists were victims of the maturing European states system and of their own archaic world-view.

Published

2012

27. Maryland Law Review

Author

Tribe, Laurence H., Tribe, Laurence H., Tribe, Laurence H., and Tribe, Laurence H.

Published

2012

28. Is the Patient Protection and Affordable Care Act Constitutional?

Author

Tribe, Laurence H., Tribe, Laurence H., Pilon, Roger, Tribe, Laurence H., Tribe, Laurence H., and Pilon, Roger

Published

2011

29. Destabilized SMC5/6 complex leads to chromosome breakage syndrome with severe lung disease

Author

van der Crabben, Saskia N, Hennus, Marije P, McGregor, Grant A, Ritter, Deborah I, Nagamani, Sandesh C S, Wells, Owen S, Harakalova, Magdalena, Chinn, Ivan K, Alt, Aaron, Vondrova, Lucie, Hochstenbach, Ron, van Montfrans, Joris M, Terheggen-Lagro, Suzanne W, van Lieshout, Stef, van Roosmalen, Markus J, Renkens, Ivo, Duran, Karen, Nijman, Isaäc J., Kloosterman, Wigard P, Hennekam, Eric, Orange, Jordan S, van Hasselt, Peter M, Wheeler, David A, Palecek, Jan J, Lehmann, Alan R, Oliver, Antony W, Pearl, Laurence H, Plon, Sharon E, Murray, Johanne M, van Haaften, Gijs, van der Crabben, Saskia N, Hennus, Marije P, McGregor, Grant A, Ritter, Deborah I, Nagamani, Sandesh C S, Wells, Owen S, Harakalova, Magdalena, Chinn, Ivan K, Alt, Aaron, Vondrova, Lucie, Hochstenbach, Ron, van Montfrans, Joris M, Terheggen-Lagro, Suzanne W, van Lieshout, Stef, van Roosmalen, Markus J, Renkens, Ivo, Duran, Karen, Nijman, Isaäc J., Kloosterman, Wigard P, Hennekam, Eric, Orange, Jordan S, van Hasselt, Peter M, Wheeler, David A, Palecek, Jan J, Lehmann, Alan R, Oliver, Antony W, Pearl, Laurence H, Plon, Sharon E, Murray, Johanne M, and van Haaften, Gijs

Published

2016

30. Visual Prognosis in USH2A-Associated Retinitis Pigmentosa Is Worse for Patients with Usher Syndrome Type IIa Than for Those with Nonsyndromic Retinitis Pigmentosa

Author

Pierrache, Laurence H M, Hartel, Bas P, van Wijk, Erwin, Meester-Smoor, Magda A, Cremers, Frans P M, de Baere, Elfride, de Zaeytijd, Julie, van Schooneveld, Mary J, Cremers, Cor W R J, Dagnelie, Gislin, Hoyng, Carel B, Bergen, Arthur A, Leroy, Bart P, Pennings, Ronald J E, van den Born, L Ingeborgh, Klaver, Caroline C W, Pierrache, Laurence H M, Hartel, Bas P, van Wijk, Erwin, Meester-Smoor, Magda A, Cremers, Frans P M, de Baere, Elfride, de Zaeytijd, Julie, van Schooneveld, Mary J, Cremers, Cor W R J, Dagnelie, Gislin, Hoyng, Carel B, Bergen, Arthur A, Leroy, Bart P, Pennings, Ronald J E, van den Born, L Ingeborgh, and Klaver, Caroline C W

Abstract

PURPOSE: USH2A mutations are an important cause of retinitis pigmentosa (RP) with or without congenital sensorineural hearing impairment. We studied genotype-phenotype correlations and compared visual prognosis in Usher syndrome type IIa and nonsyndromic RP.DESIGN: Clinic-based, longitudinal, multicenter study.PARTICIPANTS: Consecutive patients with Usher syndrome type IIa (n = 152) and nonsyndromic RP (n = 73) resulting from USH2A mutations from ophthalmogenetic clinics in the Netherlands and Belgium.METHODS: Data on clinical characteristics, visual acuity, visual field measurements, retinal imaging, and electrophysiologic features were extracted from medical charts over a mean follow-up of 9 years. Cumulative lifetime risks of low vision and blindness were estimated using Kaplan-Meier survival analysis.MAIN OUTCOME MEASURES: Low vision and blindness.RESULTS: Participant groups had similar distributions of gender (48% vs. 45% males in Usher syndrome type IIa vs. nonsydromic RP; P = 0.8), ethnicity (97% vs. 99% European; P = 0.3), and median follow-up time (6.5 years vs. 3 years; P = 0.3). Usher syndrome type IIa patients demonstrated symptoms at a younger age (median age, 15 years vs. 25 years; P < 0.001), were diagnosed earlier (median age, 26 years vs. 36.5 years; P < 0.001), and became visually impaired 13 years earlier (median age, 41 years vs. 54 years; P < 0.001) based on VF and 18 years earlier based on VA (median age, 54 years vs. 72 years; P < 0.001) than nonsyndromic RP patients. The presence of 2 truncating mutations in USH2A was associated mostly with the syndromic phenotype, whereas other combinations were present in both groups. We found novel variants in Usher syndrome type IIa (25%) and nonsyndromic RP (19%): 29 missense mutations, 10 indels, 14 nonsense mutations, 9 frameshift mutations, and 5 splice-site mutations.CONCLUSIONS: Most patients with USH2A-associated RP have severe visual impairm

Published

2016

31. Destabilized SMC5/6 complex leads to chromosome breakage syndrome with severe lung disease

Author

Metabole ziekten patientenzorg, Intensive care patientenzorg, Other research (not in main researchprogram), Infection & Immunity, Cardiologie Arts-onderzoekers, Genetica Sectie Genoomdiagnostiek, Brain, Immuno/reuma patientenzorg, Child Health, Genetica, CMM Groep Kloosterman, Genetica Groep Van Haaften, CMM Groep Cuppen, Cancer, Genetica Medische Informatica, Genetica Klinische Genetica, CMM Sectie Genomics and Bioinformatics, van der Crabben, Saskia N, Hennus, Marije P, McGregor, Grant A, Ritter, Deborah I, Nagamani, Sandesh C S, Wells, Owen S, Harakalova, Magdalena, Chinn, Ivan K, Alt, Aaron, Vondrova, Lucie, Hochstenbach, Ron, van Montfrans, Joris M, Terheggen-Lagro, Suzanne W, van Lieshout, Stef, van Roosmalen, Markus J, Renkens, Ivo, Duran, Karen, Nijman, Isaäc J., Kloosterman, Wigard P, Hennekam, Eric, Orange, Jordan S, van Hasselt, Peter M, Wheeler, David A, Palecek, Jan J, Lehmann, Alan R, Oliver, Antony W, Pearl, Laurence H, Plon, Sharon E, Murray, Johanne M, van Haaften, Gijs, Metabole ziekten patientenzorg, Intensive care patientenzorg, Other research (not in main researchprogram), Infection & Immunity, Cardiologie Arts-onderzoekers, Genetica Sectie Genoomdiagnostiek, Brain, Immuno/reuma patientenzorg, Child Health, Genetica, CMM Groep Kloosterman, Genetica Groep Van Haaften, CMM Groep Cuppen, Cancer, Genetica Medische Informatica, Genetica Klinische Genetica, CMM Sectie Genomics and Bioinformatics, van der Crabben, Saskia N, Hennus, Marije P, McGregor, Grant A, Ritter, Deborah I, Nagamani, Sandesh C S, Wells, Owen S, Harakalova, Magdalena, Chinn, Ivan K, Alt, Aaron, Vondrova, Lucie, Hochstenbach, Ron, van Montfrans, Joris M, Terheggen-Lagro, Suzanne W, van Lieshout, Stef, van Roosmalen, Markus J, Renkens, Ivo, Duran, Karen, Nijman, Isaäc J., Kloosterman, Wigard P, Hennekam, Eric, Orange, Jordan S, van Hasselt, Peter M, Wheeler, David A, Palecek, Jan J, Lehmann, Alan R, Oliver, Antony W, Pearl, Laurence H, Plon, Sharon E, Murray, Johanne M, and van Haaften, Gijs

Published

2016

32. Mice Lacking Serotonin 2C Receptors Have increased Affective Responses to Aversive Stimuli.

Author

Bonasera, Stephen J, Bonasera, Stephen J, Schenk, A Katrin, Luxenberg, Evan J, Wang, Xidao, Basbaum, Allan, Tecott, Laurence H, Bonasera, Stephen J, Bonasera, Stephen J, Schenk, A Katrin, Luxenberg, Evan J, Wang, Xidao, Basbaum, Allan, and Tecott, Laurence H

Abstract

Although central serotonergic systems are known to influence responses to noxious stimuli, mechanisms underlying serotonergic modulation of pain responses are unclear. We proposed that serotonin 2C receptors (5-HT2CRs), which are expressed within brain regions implicated in sensory and affective responses to pain, contribute to the serotonergic modulation of pain responses. In mice constitutively lacking 5-HT2CRs (2CKO mice) we found normal baseline sensory responses to noxious thermal, mechanical and chemical stimuli. In contrast, 2CKO mice exhibited a selective enhancement of affect-related ultrasonic afterdischarge vocalizations in response to footshock. Enhanced affect-related responses to noxious stimuli were also exhibited by 2CKO mice in a fear-sensitized startle assay. The extent to which a brief series of unconditioned footshocks produced enhancement of acoustic startle responses was markedly increased in 2CKO mice. As mesolimbic dopamine pathways influence affective responses to noxious stimuli, and these pathways are disinhibited in 2CKO mice, we examined the sensitivity of footshock-induced enhancement of startle to dopamine receptor blockade. Systemic administration of the dopamine D2/D3 receptor antagonist raclopride selectively reduced footshock-induced enhancement of startle without influencing baseline acoustic startle responses. We propose that 5-HT2CRs regulate affective behavioral responses to unconditioned aversive stimuli through mechanisms involving the disinhibition of ascending dopaminergic pathways.

Published

2015

33. CHARACTERIZATION AND TARGETING OF THE MULTIPLE DNA SECONDARY STRUCTURES IN THE KRAS PROXIMAL PROMOTER TO MODULATE GENE EXPRESSION

Author

Hurley, Laurence H., Yang, Danzhou, Wondrak, Georg, Sun, Daekyu, Kaiser, Christine Elizabeth, Hurley, Laurence H., Yang, Danzhou, Wondrak, Georg, Sun, Daekyu, and Kaiser, Christine Elizabeth

Abstract

KRAS is a well-validated drug target for anti-cancer therapy, yet no clinically useful drugs that directly inhibit its function currently exist. We aim to target KRAS at the transcriptional level, through DNA secondary structures.

Published

2015

34. Characterization and Molecular Targeting of a Mechanosensor Mechanism Controlled By the G-Quadruplex/I-Motif Molecular Switch in the MYC Promoter NHE III₁

Author

Sun, Daekyu, Smith, Cathy, Rimsza, Lisa, Hurley, Laurence H., Sutherland, Caleb Daniel, Sun, Daekyu, Smith, Cathy, Rimsza, Lisa, Hurley, Laurence H., and Sutherland, Caleb Daniel

Abstract

MYC is overexpressed in most types of tumors, but a means to selectively decrease its expression is yet to be found. Our recent findings on modulation of BCL2 gene expression through protein interactions with the BCL2 i-motif have provided a basis for further investigation of MYC gene control. It is proposed that the MYC i-motif could function by a similar molecular switch mechanism as in BCL2.Binding sites for heterogeneous nuclear ribonucleoprotein K (hnRNP K) within the MYC promoter also exist in the i-motif-forming sequence. Circular dichroism and bromine footprinting confirmed that this DNA sequence is able to form an i-motif, and systematic mutation of the cytosine residues in this sequence has revealed a 5:5:5 loop configuration. Indeed, all loops of the i-motif, when folded into a 5:5:5 loop configuration, contain the hnRNP K consensus sequence (CCCT). Previous studies show that hnRNP K binds to this i-motif-forming sequence, but it was assumed to be single-stranded. Binding studies revealed that hnRNP K has more binding affinity to its consensus sequence in the i-motif compared to a mutant sequence where the i-motif cannot form. Further investigation of the MYC promoter revealed an additional two runs of cytosine seven bases downstream of the MYC i-motif. Biophysical studies showed that the additional two runs were not involved in i-motif formation, however recent studies describe their importance for transcriptional activation. We found that hnRNP K preferred the longer 5CT sequence compared to the i-motif forming 4CT sequence when using a competitive binding assay. Utilizing luciferase reporters containing either the 4CT or 5CT sequence validated that hnRNP K required both the i-motif and 5th CT element for maximum transcriptional activation. Competition binding studies and bromine footprinting showed that hnRNP K bound to the downstream 5th CT element and the central and lateral loops of the i-motif.Additionally, we found that co-overexpression of Sp1 an

Published

2015

35. Axonal control of the adult neural stem cell niche.

Author

Tong, Cheuk Ka, Tong, Cheuk Ka, Chen, Jiadong, Cebrián-Silla, Arantxa, Mirzadeh, Zaman, Obernier, Kirsten, Guinto, Cristina D, Tecott, Laurence H, García-Verdugo, Jose Manuel, Kriegstein, Arnold, Alvarez-Buylla, Arturo, Tong, Cheuk Ka, Tong, Cheuk Ka, Chen, Jiadong, Cebrián-Silla, Arantxa, Mirzadeh, Zaman, Obernier, Kirsten, Guinto, Cristina D, Tecott, Laurence H, García-Verdugo, Jose Manuel, Kriegstein, Arnold, and Alvarez-Buylla, Arturo

Abstract

The ventricular-subventricular zone (V-SVZ) is an extensive germinal niche containing neural stem cells (NSCs) in the walls of the lateral ventricles of the adult brain. How the adult brain's neural activity influences the behavior of adult NSCs remains largely unknown. We show that serotonergic (5HT) axons originating from a small group of neurons in the raphe form an extensive plexus on most of the ventricular walls. Electron microscopy revealed intimate contacts between 5HT axons and NSCs (B1) or ependymal cells (E1) and these cells were labeled by a transsynaptic viral tracer injected into the raphe. B1 cells express the 5HT receptors 2C and 5A. Electrophysiology showed that activation of these receptors in B1 cells induced small inward currents. Intraventricular infusion of 5HT2C agonist or antagonist increased or decreased V-SVZ proliferation, respectively. These results indicate that supraependymal 5HT axons directly interact with NSCs to regulate neurogenesis via 5HT2C.

Published

2014

36. Active surveillance for clinically localized prostate cancer:a systematic review

Author

Thomsen, Frederik B, Brasso, Klaus, Klotz, Laurence H, Røder, M Andreas, Berg, Kasper D, Iversen, Peter, Thomsen, Frederik B, Brasso, Klaus, Klotz, Laurence H, Røder, M Andreas, Berg, Kasper D, and Iversen, Peter

Abstract

Active surveillance (AS) has been introduced as an observational strategy to delay or avoid curative treatment without compromising long-term cancer-specific survival. The 10 studies included in this review, published between 2008 and 2013, generally agreed upon patients selection for the AS strategy and how they should be managed within the program. However, uncertainties persists concerning optimal patient selection and reliable progression criteria, as well as the long-term safety of AS.

Published

2014

37. Moving a randomized clinical trial into an observational cohort.

Author

Goodman, Phyllis J, Goodman, Phyllis J, Hartline, Jo Ann, Tangen, Catherine M, Crowley, John J, Minasian, Lori M, Klein, Eric A, Cook, Elise D, Darke, Amy K, Arnold, Kathryn B, Anderson, Karen, Yee, Monica, Meyskens, Frank L, Baker, Laurence H, Goodman, Phyllis J, Goodman, Phyllis J, Hartline, Jo Ann, Tangen, Catherine M, Crowley, John J, Minasian, Lori M, Klein, Eric A, Cook, Elise D, Darke, Amy K, Arnold, Kathryn B, Anderson, Karen, Yee, Monica, Meyskens, Frank L, and Baker, Laurence H

Abstract

The Selenium and Vitamin E Cancer Prevention Trial (SELECT) was a randomized, double-blind, placebo-controlled prostate cancer prevention study funded by the National Cancer Institute (NCI) and conducted by the Southwest Oncology Group (SWOG). A total of 35,533 men were assigned randomly to one of the four treatment groups (vitamin E + placebo, selenium + placebo, vitamin E + selenium, and placebo + placebo). The independent Data and Safety Monitoring Committee (DSMC) recommended the discontinuation of study supplements because of the lack of efficacy for risk reduction and because futility analyses demonstrated no possibility of benefit of the supplements to the anticipated degree (25% reduction in prostate cancer incidence) with additional follow-up. Study leadership agreed that the randomized trial should be terminated but believed that the cohort should be maintained and followed as the additional follow-up would contribute important information to the understanding of the biologic consequences of the intervention. Since the participants no longer needed to be seen in person to assess acute toxicities or to be given study supplements, it was determined that the most efficient and cost-effective way to follow them was via a central coordinated effort.A number of changes were necessary at the local Study Sites and SELECT Statistical Center to transition to following participants via a Central Coordinating Center. We describe the transition process from a randomized clinical trial to the observational Centralized Follow-Up (CFU) study.The process of transitioning SELECT, implemented at more than 400 Study Sites across the United States, Canada, and Puerto Rico, entailed many critical decisions and actions including updates to online documents such as the SELECT Workbench and Study Manual, a protocol amendment, reorganization of the Statistical Center, creation of a Transition Committee, development of materials for SELECT Study Sites, development of procedures to c

Published

2013

38. Impact of serotonin (5-HT)2C receptors on executive control processes.

Author

Pennanen, Luis, Pennanen, Luis, van der Hart, Marieke, Yu, Lisa, Tecott, Laurence H, Pennanen, Luis, Pennanen, Luis, van der Hart, Marieke, Yu, Lisa, and Tecott, Laurence H

Abstract

Although the serotonin (5-hydroxytryptamine, 5-HT) neurotransmitter system has been implicated in modulating executive control processes such as attention, response inhibition, and behavioral flexibility, the contributions of particular serotonin receptors remain unclear. Here, using operant-based behavioral paradigms, we demonstrate that mice with genetically ablated 5-HT2C receptors (2CKO mice) display deficits in executive functions. 2CKO mice were impaired in the acquisition of a visuospatial attention task as assessed in the 5-choice serial reaction time task (5-CSRTT). In this task, 2CKO mice exhibited marked impairment of attentional processes, with normal response inhibition. We assessed dynamic changes in neurotransmitter levels within the nucleus accumbens (NAc) by in vivo microdialysis in task-performing animals. Extracellular dopamine concentrations were elevated in the NAc of 2CKO mice during task performance, indicating that 5-HT2C receptors impact dopamine homeostasis during a visuospatial attention task. These findings raise the possibility that disinhibition of mesolimbic dopamine pathways contributes to impaired attention and perturbed task performance in 2CKO mice. Additionally, in a spatial reversal learning task, 2CKO mice failed to improve their performance over a series of reversals, indicating that intact 5-HT2C receptor signaling is required to accurately respond to repeated changes in reward contingencies. In contrast to the 2CKO phenotype in the 5-CSRTT, wild-type mice treated with the 5-HT2C receptor antagonist SB242084 exhibited diminished response inhibition, suggesting differing effects of acute pharmacological blockade and constitutive loss of 5-HT2C receptor activity. Altogether, these findings provide insights into the serotonergic regulation of executive control processes and suggest that impaired 5-HT2C receptor signaling during development may predispose to executive function disorders.

Published

2013

39. Vitamin E and the risk of prostate cancer: Updated results of the Selenium and Vitamin E Cancer Prevention Trial (SELECT).

Author

Klein, Eric A, Klein, Eric A, Thompson, Ian, Tangen, Catherine M, Lucia, M Scott, Goodman, Phyllis, Minasian, Lori M, Ford, Leslie G, Parnes, Howard L, Gaziano, J Michael, Karp, Daniel D, Lieber, Michael M, Walther, Philip John, Parsons, J Kellogg, Chin, Joseph, Darke, Amy K, Lippman, Scott Michael, Goodman, Gary E, Meyskens, Frank L, Baker, Laurence H, Klein, Eric A, Klein, Eric A, Thompson, Ian, Tangen, Catherine M, Lucia, M Scott, Goodman, Phyllis, Minasian, Lori M, Ford, Leslie G, Parnes, Howard L, Gaziano, J Michael, Karp, Daniel D, Lieber, Michael M, Walther, Philip John, Parsons, J Kellogg, Chin, Joseph, Darke, Amy K, Lippman, Scott Michael, Goodman, Gary E, Meyskens, Frank L, and Baker, Laurence H

Abstract

7 Background: The initial report of the Selenium and Vitamin E Cancer Prevention Trial (SELECT) found no reduction in risk of prostate cancer with either selenium or vitamin E supplements but a non-statistically significant increase in prostate cancer risk with vitamin E. Longer follow-up and more prostate cancer events provide further insight into the relationship of vitamin E and prostate cancer.SELECT randomized 35,533 men from 427 study sites in the United States, Canada and Puerto Rico in a double-blind manner between August 22, 2001 and June 24, 2004. Eligible men were 50 years or older (African Americans) or 55 years or older (all others) with a PSA <4.0 ng/mL and a digital rectal examination not suspicious for prostate cancer. Included in the analysis are 34,887 men randomly assigned to one of four treatment groups: selenium (n=8752), vitamin E (n=8737), both agents (n=8702), or placebo (n=8696). Data reflect the final data collected by the study sites on their participants through July 5, 2011.This report includes 54,464 additional person-years of follow-up since the primary report. Hazard ratios (99% confidence intervals [CI]) and numbers of prostate cancers were 1.17 (99% CI 1.004-1.36, p=.008, n=620) for vitamin E, 1.09 (99% CI 0.93-1.27, p=.18, n=575) for selenium, 1.05 (99%CI 0.89-1.22, p=.46, n=555) for selenium + vitamin E vs. 1.00 (n=529) for placebo. The absolute increase in risk compared with placebo for vitamin E, selenium and the combination were 1.6, 0.9 and 0.4 cases of prostate cancer per 1,000 person-years.Dietary supplementation with Vitamin E significantly increases the risk of prostate cancer among healthy men.

Published

2012

40. Active surveillance for prostate cancer: a systematic review of the literature.

Author

Dall'Era, Marc A, Dall'Era, Marc A, Albertsen, Peter C, Bangma, Christopher, Carroll, Peter R, Carter, H Ballentine, Cooperberg, Matthew R, Freedland, Stephen J, Klotz, Laurence H, Parker, Christopher, Soloway, Mark S, Dall'Era, Marc A, Dall'Era, Marc A, Albertsen, Peter C, Bangma, Christopher, Carroll, Peter R, Carter, H Ballentine, Cooperberg, Matthew R, Freedland, Stephen J, Klotz, Laurence H, Parker, Christopher, and Soloway, Mark S

Abstract

ContextProstate cancer (PCa) remains an increasingly common malignancy worldwide. The optimal management of clinically localized, early-stage disease remains unknown, and profound quality of life issues surround PCa interventions.ObjectiveTo systematically summarize the current literature on the management of low-risk PCa with active surveillance (AS), with a focus on patient selection, outcomes, and future research needs.Evidence acquisitionA comprehensive search of the PubMed and Embase databases from 1980 to 2011 was performed to identify studies pertaining to AS for PCa. The search terms used included prostate cancer and active surveillance or conservative management or watchful waiting or expectant management. Selected studies for outcomes analysis had to provide a comprehensive description of entry characteristics, criteria for surveillance, and indicators for further intervention.Evidence synthesisData from seven large AS series were reviewed. Inclusion criteria for surveillance vary among studies, and eligibility therefore varies considerably (4-82%). PCa-specific mortality remains low (0-1%), with the longest published median follow-up being 6.8 yr. Up to one-third of patients receive secondary therapy after a median of about 2.5 yr of surveillance. Surveillance protocols and triggers for intervention vary among institutions. Most patients are treated for histologic reclassification (27-100%) or prostate-specific antigen doubling time <3 yr (13-48%), while 7-13% are treated with no evidence of progression. Repeat prostate biopsy with a minimum of 12 cores appears to be important for monitoring patients for changes in tumor histology over time.ConclusionsAS for PCa offers an opportunity to limit intervention to patients who will likely benefit the most from radical treatment. This approach confers a low risk of disease-specific mortality in the short to intermediate term. An early, confirmatory biopsy is essential for limiting the risk of underestimating

Published

2012

41. Minor structural modifications to alchemix influence mechanism of action and pharmacological activity

Author

Abdallah, Qasem M. A., Phillips, Roger M., Johansson, Fredrik, Helleday, Thomas, Cosentino, Laura, Abdel-Rahman, Hamdy, Etzad, Jasarat, Wheelhouse, Richard T., Kiakos, Konstantinos, Bingham, John P., Hartley, John A., Patterson, Laurence H., Pors, Klaus, Abdallah, Qasem M. A., Phillips, Roger M., Johansson, Fredrik, Helleday, Thomas, Cosentino, Laura, Abdel-Rahman, Hamdy, Etzad, Jasarat, Wheelhouse, Richard T., Kiakos, Konstantinos, Bingham, John P., Hartley, John A., Patterson, Laurence H., and Pors, Klaus

Abstract

Alchemix is an exemplar of a class of anthraquinone with efficacy against multidrug resistant tumours. We have explored further the mechanism of action of alchemix and investigated the effect of extending its side arm bearing the alkylating functionality with regard to DNA binding and activity against multidrug resistant cancer cells. Increasing the distance between the intercalating chromophore and the alkylating functionality of ICT2901 (propyl), ICT2902 (butyl) and ICT2903 (pentyl), led to a higher number of DNA alkylation sites, more potent topoisomerase II inhibition and generated more apoptotic and necrotic cells when analysed in p53-proficient HCT116 cells. Intriguingly, alchemix, the compound with the shortest distance between its intercalative chromophore and alkylating functionality (ethyl), did not conform to this SAR. A different toxicity pattern against DNA repair defective CHO cell lines as well as arrest of cells in Cl supports a somewhat distinct mode of action by alchemix compared with its analogues. Importantly, both alchemix and ICT2901 demonstrated greater cytotoxic activity against anthraquinone-resistant MCF-7/adr cells than wild-type MCF-7 cells. Subtle synthetic modification in this anthraquinone series has led to significant changes to the stability of DNA-compound complexes and cellular activity. Given that the failure of chemotherapy in the clinic is often associated with MDR, the results of both alchemix and ICT2901 represent important advances towards improved therapies., AuthorCount:13

Published

2012

42. An investigation of the MCDEC research and development program prioritization process.

Author

NA, Nelson, Laurence H., NA, and Nelson, Laurence H.

Abstract

http://archive.org/details/aninvestigationo1094519409, NA, NA

Published

2012

43. When progressive disease does not mean treatment failure: reconsidering the criteria for progression.

Author

Oxnard, Geoffrey R, Oxnard, Geoffrey R, Morris, Michael J, Hodi, F Stephen, Baker, Laurence H, Kris, Mark G, Venook, Alan P, Schwartz, Lawrence H, Oxnard, Geoffrey R, Oxnard, Geoffrey R, Morris, Michael J, Hodi, F Stephen, Baker, Laurence H, Kris, Mark G, Venook, Alan P, and Schwartz, Lawrence H

Abstract

Although progression-based endpoints, such as progression-free survival, are often key clinical trial endpoints for anticancer agents, the clinical meaning of "objective progression" is much less certain. As scrutiny of progression-based endpoints in clinical trials increases, it should be remembered that the Response Evaluation Criteria In Solid Tumors (RECIST) progression criteria were not developed as a surrogate for survival. Now that progression-free survival has come to be an increasingly important trial endpoint, the criteria that define progression deserve critical evaluation to determine whether alternate definitions of progression might facilitate the development of stronger surrogate endpoints and more meaningful trial results. In this commentary, we review the genesis of the criteria for progression, highlight recent data that question their value as a marker of treatment failure, and advocate for several research strategies that could lay the groundwork for a clinically validated definition of disease progression in solid tumor oncology.

Published

2012

44. Serotonin 5-HT2C receptor knockout mice: Autoradiographic analysis of multiple serotonin receptors

Author

López-Giménez, Juan F., Tecott, Laurence H., Palacios, José M., Mengod Los Arcos, Guadalupe, Vilaró, Maria Teresa, López-Giménez, Juan F., Tecott, Laurence H., Palacios, José M., Mengod Los Arcos, Guadalupe, and Vilaró, Maria Teresa

Abstract

Quantitative receptor autoradiography was used to study possible alterations of the densities of multiple serotonin (5-HT) receptor subtypes and of serotonin transporter in the brain of 5-HT2C receptor knockout mice. The radioligands employed were [3H]citalopram, [3H]WAY100,635, [3H]8-OH-DPAT, [3H]GR125743, [3H]sumatriptan, [3H]MDL100,907, [125I](=)DOI, [3H]mesulergine, [3H]5-HT, [3H]GR113808, and [3H]5-CT. As expected, radioligands that label 5-HT2C receptors showed a complete absence of labeling in mutant mice choroid plexus and significantly reduced densities in other brain regions expressing 5-HT2C receptors. With the rest of the radioligands, no significant alterations in the densities of labeled sites were found in any brain region. In situ hybridization showed no changes in 5-HT2A receptor and serotonin transporter mRNA levels, whereas 5-HT2C receptor mRNA levels were reduced in certain brain regions. The present results indicate that the mouse serotonergic system does not exhibit compensatory up- or down-regulation of the majority of its components (serotonin transporter and most 5-HT receptor subtypes) in response to the absence of 5-HT2C receptors. © 2002 Wiley-liss, Inc.

Published

2011

45. Evidence for a remodelling of DNA-PK upon autophosphorylation from electron microscopy studies

Author

Morris, Edward P., Rivera-Calzada, Angel, Fonseca, Paula C.A. de, Llorca, Óscar, Pearl, Laurence H., Spagnolo, Laura, Morris, Edward P., Rivera-Calzada, Angel, Fonseca, Paula C.A. de, Llorca, Óscar, Pearl, Laurence H., and Spagnolo, Laura

Abstract

The multi-subunit DNA-dependent protein kinase (DNA-PK), a crucial player in DNA repair by non-homologous end-joining in higher eukaryotes, consists of a catalytic subunit (DNA-PKcs) and the Ku heterodimer. Ku recruits DNA-PKcs to double-strand breaks, where DNA-PK assembles prior to DNA repair. The interaction of DNA-PK with DNA is regulated via autophosphorylation. Recent SAXS data addressed the conformational changes occurring in the purified catalytic subunit upon autophosphorylation. Here, we present the first structural analysis of the effects of autophosphorylation on the trimeric DNA-PK enzyme, performed by electron microscopy and single particle analysis. We observe a considerable degree of heterogeneity in the autophosphorylated material, which we resolved into subpopulations of intact complex, and separate DNA-PKcs and Ku, by using multivariate statistical analysis and multi-reference alignment on a partitioned particle image data set. The proportion of dimeric oligomers was reduced compared to non-phosphorylated complex, and those dimers remaining showed a substantial variation in mutual monomer orientation. Together, our data indicate a substantial remodelling of DNA-PK holo-enzyme upon autophosphorylation, which is crucial to the release of protein factors from a repaired DNA double-strand break.

Published

2011

46. Serotonin regulates pancreatic beta cell mass during pregnancy.

Author

Kim, Hail, Kim, Hail, Toyofuku, Yukiko, Lynn, Francis C, Chak, Eric, Uchida, Toyoyoshi, Mizukami, Hiroki, Fujitani, Yoshio, Kawamori, Ryuzo, Miyatsuka, Takeshi, Kosaka, Yasuhiro, Yang, Katherine, Honig, Gerard, van der Hart, Marieke, Kishimoto, Nina, Wang, Juehu, Yagihashi, Soroku, Tecott, Laurence H, Watada, Hirotaka, German, Michael S, Kim, Hail, Kim, Hail, Toyofuku, Yukiko, Lynn, Francis C, Chak, Eric, Uchida, Toyoyoshi, Mizukami, Hiroki, Fujitani, Yoshio, Kawamori, Ryuzo, Miyatsuka, Takeshi, Kosaka, Yasuhiro, Yang, Katherine, Honig, Gerard, van der Hart, Marieke, Kishimoto, Nina, Wang, Juehu, Yagihashi, Soroku, Tecott, Laurence H, Watada, Hirotaka, and German, Michael S

Abstract

During pregnancy, the energy requirements of the fetus impose changes in maternal metabolism. Increasing insulin resistance in the mother maintains nutrient flow to the growing fetus, whereas prolactin and placental lactogen counterbalance this resistance and prevent maternal hyperglycemia by driving expansion of the maternal population of insulin-producing beta cells. However, the exact mechanisms by which the lactogenic hormones drive beta cell expansion remain uncertain. Here we show that serotonin acts downstream of lactogen signaling to stimulate beta cell proliferation. Expression of serotonin synthetic enzyme tryptophan hydroxylase-1 (Tph1) and serotonin production rose sharply in beta cells during pregnancy or after treatment with lactogens in vitro. Inhibition of serotonin synthesis by dietary tryptophan restriction or Tph inhibition blocked beta cell expansion and induced glucose intolerance in pregnant mice without affecting insulin sensitivity. Expression of the G alpha(q)-linked serotonin receptor 5-hydroxytryptamine receptor-2b (Htr2b) in maternal islets increased during pregnancy and normalized just before parturition, whereas expression of the G alpha(i)-linked receptor Htr1d increased at the end of pregnancy and postpartum. Blocking Htr2b signaling in pregnant mice also blocked beta cell expansion and caused glucose intolerance. These studies reveal an integrated signaling pathway linking beta cell mass to anticipated insulin need during pregnancy. Modulators of this pathway, including medications and diet, may affect the risk of gestational diabetes.

Published

2010

47. Enhanced food anticipatory activity associated with enhanced activation of extrahypothalamic neural pathways in serotonin2C receptor null mutant mice.

Author

Hsu, Jennifer L, Hsu, Jennifer L, Yu, Lisa, Sullivan, Elinor, Bowman, Melodi, Mistlberger, Ralph E, Tecott, Laurence H, Hsu, Jennifer L, Hsu, Jennifer L, Yu, Lisa, Sullivan, Elinor, Bowman, Melodi, Mistlberger, Ralph E, and Tecott, Laurence H

Abstract

The ability to entrain circadian rhythms to food availability is important for survival. Food-entrained circadian rhythms are characterized by increased locomotor activity in anticipation of food availability (food anticipatory activity). However, the molecular components and neural circuitry underlying the regulation of food anticipatory activity remain unclear. Here we show that serotonin(2C) receptor (5-HT2CR) null mutant mice subjected to a daytime restricted feeding schedule exhibit enhanced food anticipatory activity compared to wild-type littermates, without phenotypic differences in the impact of restricted feeding on food consumption, body weight loss, or blood glucose levels. Moreover, we show that the enhanced food anticipatory activity in 5-HT2CR null mutant mice develops independent of external light cues and persists during two days of total food deprivation, indicating that food anticipatory activity in 5-HT2CR null mutant mice reflects the locomotor output of a food-entrainable oscillator. Whereas restricted feeding induces c-fos expression to a similar extent in hypothalamic nuclei of wild-type and null mutant animals, it produces enhanced expression in the nucleus accumbens and other extrahypothalamic regions of null mutant mice relative to wild-type subjects. These data suggest that 5-HT2CRs gate food anticipatory activity through mechanisms involving extrahypothalamic neural pathways.

Published

2010

48. Small Town Insurgency: The Struggle for Information Dominance to Reduce Gang Violence

Author

NAVAL POSTGRADUATE SCHOOL MONTEREY CA, Arnold, Laurence H., O'Gwin, Christopher W., Vickers, Jeremy S., NAVAL POSTGRADUATE SCHOOL MONTEREY CA, Arnold, Laurence H., O'Gwin, Christopher W., and Vickers, Jeremy S.

Abstract

Since 2006, the gang related homicide rate in Salinas, California has quadrupled. As of 2009 the homicide rate associated with gang activity far exceeds those of much larger cities such as San Francisco, San Jose, and even Los Angeles, California. This report examines this negative trend through the lens of counterinsurgency, since gangs exhibit many similarities in structure and tactics to insurgent groups. Accordingly, this thesis capitalizes on the diverse academic theories available to the study of counterinsurgencies. While the common narrative for an effective counterinsurgency campaign focuses on the importance of information dominance, there has been little research into component factors that might either promote, or inhibit, the flow of information that is also critical in combating the American street gang phenomenon. In reality, gangs exist because of an information advantage bestowed upon them by the population. Thus, we postulate that two factors, information volume and information processing, mutually contribute to information dominance with respect to a counter-gang strategy. Through comparative analysis, our research suggests that improving relationships between the population and the government encourages more communication about gang activities. Additionally, improving communication structures within the government enhances information processing. Combined, these two factors reduce the gang's information advantage., The original document contains color images.

Published

2010

49. Swe1Wee1-dependent tyrosine phosphorylation of Hsp90 regulates distinct facets of chaperone function

Author

Mollapour, Mehdi, Tsutsumi, Shinji, Donnelly, Alison C., Beebe, Kristin, Tokita, Mari J., Lee, Min-Jung, Lee, Sunmin, Morra, Giulia, Bourboulia, Dimitra, Scroggins, Bradley T., Colombo, Giorgio, Blagg, Brian S., Panaretou, Barry, Stetler-Stevenson, William G., Trepel, Jane B., Piper, Peter W., Prodromou, Chrisostomos, Pearl, Laurence H., Neckers, Len, Mollapour, Mehdi, Tsutsumi, Shinji, Donnelly, Alison C., Beebe, Kristin, Tokita, Mari J., Lee, Min-Jung, Lee, Sunmin, Morra, Giulia, Bourboulia, Dimitra, Scroggins, Bradley T., Colombo, Giorgio, Blagg, Brian S., Panaretou, Barry, Stetler-Stevenson, William G., Trepel, Jane B., Piper, Peter W., Prodromou, Chrisostomos, Pearl, Laurence H., and Neckers, Len

Abstract

Saccharomyces WEE1 (Swe1), the only “true” tyrosine kinase in budding yeast, is an Hsp90 client protein. Here we show that Swe1Wee1 phosphorylates a conserved tyrosine residue (Y24 in yeast Hsp90 and Y38 in human Hsp90?) in the N domain of Hsp90. Phosphorylation is cell-cycle associated and modulates the ability of Hsp90 to chaperone a selected clientele, including v-Src and several other kinases. Nonphosphorylatable mutants have normal ATPase activity, support yeast viability, and productively chaperone the Hsp90 client glucocorticoid receptor. Deletion of SWE1 in yeast increases Hsp90 binding to its inhibitor geldanamycin, and pharmacologic inhibition/silencing of Wee1 sensitizes cancer cells to Hsp90 inhibitor-induced apoptosis. These findings demonstrate that Hsp90 chaperoning of distinct client proteins is differentially regulated by specific posttranslational modification of a unique subcellular pool of the chaperone, and they provide a strategy to increase the cellular potency of Hsp90 inhibitors.

Published

2010

50. Defining the Role of Nucleolin on the Transcriptional Regulation of c-MYC through Modulation of the c-MYC NHE III1 Element.

Author

Hurley, Laurence H., Monks, Terrence, Vaillancourt, Richard, Parker, Roy, Sun, Daekyu, Baker, Amanda, Gonzalez, Veronica, Hurley, Laurence H., Monks, Terrence, Vaillancourt, Richard, Parker, Roy, Sun, Daekyu, Baker, Amanda, and Gonzalez, Veronica

Abstract

The activated product of the c-MYC proto-oncogene is one of the strongest known activators of carcinogenesis. It has been estimated that as many as one-seventh of all cancer deaths are associated with alterations in the c-MYC gene or its expression [1]. Therefore, understanding the regulation of c-MYC expression is a key factor in understanding carcinogenesis in many histologic classes of malignancy. The nuclease hypersensitive element (NHE) III₁ region of the c-MYC promoter has been shown to be particularly important in regulating c-MYC expression. Specifically, the formation of a G-quadruplex structure appears to promote repression of c-MYC transcription. In this dissertation, we investigate the role that nucleolin, a critical player in ribosome biogenesis and cell stress sensing, plays on the transcriptional regulation of the c-MYC promoter through its interaction with the c-MYC G-quadruplex structure. Our studies initiated with the design of a c-MYC G-quadruplex affinity column intended to trap potential c-MYC G-quadruplex-binding proteins that were then identified by LC-MS/MS. After careful examination of the literature of the list of potential c-MYC G-quadruplexbinding proteins, we realized that several of the proteins identified had been previously reported to interact directly with nucleolin. Consequently, we chose to focus our studies on nucleolin, as it could be a central regulator of the (NHE) III region. By performing chromatin immunoprecipitation in HeLa cells, we found that nucleolin indeed interacts with the c-MYC promoter region containing the NHE III₁ element. This binding activity was confirmed by both electromobility shift assay and polymerase stop assay. We provide evidence that nucleolin can induce the formation of the c-MYC G-quadruplex structure from single-stranded DNA, both in linear and circular DNA forms. We show that upon binding, nucleolin increases the stability of the c-MYC G-quadruplex structure leading to repression of c-MYC promoter

Published

2010