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449 results on '"Frantz, R"'

153. Titanium-Catalyzed Stereoselective Geminal Heterodihalogenation of β-Ketoesters

Author

Frantz, R., Hintermann, L., Perseghini, M., Broggini, D., and Togni, A.

Abstract

β-Ketoesters can be effectively monofluorinated with F-TEDA using CpTiCl3 as a catalyst. With the use of this catalyst, the extent of the competing difluorination does not reach 10%. [TiCl2(TADDOLato)] complexes catalyze the one-pot enantioselective heterodihalogenation of β-ketoesters with F-TEDA and NCS to afford α-chloro-α-fluoro-β-ketoesters in moderate to good yields. The sequence of addition of the halogenating agents determines the sense of chiral induction.

Published
2003

156. Patterns of Luteinizing Hormone in Serum Following Administration of Stalk-Median Eminence Extracts to Rhesus Monkeys1

Author

Spies, H. G., Frantz, R. C., and Niswender, G. D.

Abstract

Concentrations of luteinizing hormone (LH) were determined in serum samples collected from the femoral vein of rhesus monkeys at 5-15-min-intervals following administration of ovine stalk-median eminence extract (SMEE). Following iv injections of .02-.32 eq SMEE, a dose-related response was observed in serum LH. A marked increase in LH of 3-50 × baseline occurred within 5 min of SMEE injection. This rise in serum LH returned to baseline within 60-90 min. Chronic iv infusion of SMEE for 5-6.5 hr elicited an immediate rise in serum LH and a plateau which lasted until the infusion ceased. The increased concentrations of serum LH prompted by equivalent dosages of SMEE given at Days 5-7, 9-13, or 19-23 of the menstrual cycle or following injection of 0.5 mg of progesterone sc on days 6-12 were comparable. Antiestrogen, U-11, 100A injected sc at 0.5 mg daily on days 7-12, significantly reduced the LH released by SMEE injections. The decreased response to SMEE stimulus following antiestrogen, but not progesterone injections, suggest these compounds influence LH release via different mechanisms. In control, progesterone- and antiestro-gen-treated monkeys the iv injection of SMEE did not induce ovulation, whereas two of three “progesterone-blocked” females did ovulate following a 5-6.5 hr chronic infusion indicating the duration of LH elevation was critical.

Published
1972
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158. The Dynamic Stress-Strain Behavior in Torsion of 1100-0 Aluminum Subjected to a Sharp Increase in Strain Rate

Author

Frantz, R. A. and Duffy, J.

Abstract

A modification of the torsional split Hopkinson bar is described which superimposes a high rate of shear strain on a slower “static” rate. The static rate of 5 × 10−5 sec−1 is increased to 850 sec−1 at a predetermined value of plastic strain by the detonation of small explosive charges; the rise time of the strain-rate increment is about 10 microsec. During deformation at the dynamic rate, direct measurement is made of the excess stress above the maximum static stress attained. Results for 1100-O aluminum show that the initial response to the strain rate increment is elastic, followed by yielding behavior reminiscent in appearance to an upper yield point. The incremental stress-strain curve always lies beneath the stress-strain curve obtained entirely at the higher strain rate but approaches it asymptotically with increasing strain. It is concluded that the material behavior is a function of strain, strain rate, and strain rate history.

Published
1972
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159. The Deformation of Lead in Torsion at High Strain Rates

Author

Duffy, J., Hawley, R. H., and Frantz, R. A.

Abstract

Experiments are described in which specimens of lead are strained in torsion at high rates using the split Hopkinson bar and explosive loading. Tests were conducted at nominal strain rates of 1000 sec−1 and 5000 sec−1 as well as at “static” rates. Values of the flow stress correspond closely with those obtained in axial tests by other investigators at corresponding rates.

Published
1972
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160. DEC PDP-7/IBM 1800 HIGH SPEED INTERFACE REFERENCE MANUAL

Author

null J. A., Miller D. R., Frantz R. F., Brender J. L., and Jr. Foy

Subjects
Data processing, SIMPLE (military communications protocol), Computer science, business.industry, Transfer (computing), Interface (computing), IBM, business, Queued Telecommunications Access Method, Computer hardware, Word (computer architecture), IBM 2321 Data Cell
Abstract

The report describes an interface between an IBM 1800 computer and a DEC PDP-7 computer. It has the following features: (1) it allows the transfer of blocks of data directly from the memory of one computer to the memory of the other, at up to 125,000 words per second, in parallel with program execution; (2) it allows a program running on one machine to interact asynchronously with one running on the other through a system of 'attention interrupts'; (3) it is relatively simple to control, being symmetric to both computers; (4) it compensates automatically, in either of two modes, for the difference in word length between the PDP-7 and the 1800.

Published
1970
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161. History Effects in Polycrystalline FCC Metals Subjected to Rapid Changes in Strain Rate and Temperature.

Author

BROWN UNIV PROVIDENCE R I DEPT OF ENGINEERING, Klepaczko,J., Frantz,R. A., Duffy,J., BROWN UNIV PROVIDENCE R I DEPT OF ENGINEERING, Klepaczko,J., Frantz,R. A., and Duffy,J.

Abstract

A review is presented of available experimental data on strain rate and temperature history effects for fcc polycrystalline metals together with new experimental results on copper and lead. It is evident from all the data presented that history effects play an important role which cannot be neglected in deriving constitutive relations to describe the plastic behavior of metals. It is shown in this paper that the influence of strain or temperature on the flow stress can be divided into two parts. The initial part is due to the existing work-hardened structure at that strain level, while the second is associated with the formation history of that structure. A possible explanation for these effects lies in dynamic recovery processes which take place during the slower deformation before the imposition of the rapid change in strain rate or temperature.

Published
1974

162. The Dynamic Stress-Strain Behavior in Torsion of 1100-0 Aluminum Subjected to a Sharp Increase in Strain Rate.

Author

BROWN UNIV PROVIDENCE R I DIV OF ENGINEERING, Frantz,R. A. , Jr., Duffy,J., BROWN UNIV PROVIDENCE R I DIV OF ENGINEERING, Frantz,R. A. , Jr., and Duffy,J.

Abstract

A modification of the torsional split Hopkinson bar is described which superimposes a high rate of shear strain on a slower 'static' rate. The 'static' rate of 0.00005/sec is increased to 850/sec at a predetermined value of plastic strain by the detonation of small explosive charges; the rise time of the strain rate increment is about 10 microseconds. During deformation at the dynamic rate, direct measurement is made of the excess stress above the maximum static stress attained. Results for 1100-0 aluminum show that the initial response to the strain rate increment is elastic, followed by yielding behavior reminiscent in appearance to an upper yield point. The magnitude of the stress measured at this yield point is always less than the stress obtained at the same strain in a wholly dynamic test; as the stress-strain curve asymptotically. It is concluded that the material behavior is a function of strain, strain rate and strain rate history. (Author)

Published
1971

166. Sildenafil citrate therapy for pulmonary arterial hypertension (vol 353, pg 2148, 2005)

Author

Manes, A., Seeger, W., Fijalkowska, A., Kramer, M. R., Peacock, A. J., Sitbon, O., Al-Hiti, H., Pulido, T., Ben-Dov, I., Frost, A. E., Zwicke, D. L., Shapiro, S. M., Keogh, A., Ickinger, C., Frantz, R. P., Hill, N. S., Ouduz, R. J., Karlocai, K., Yu, C. M., Boonstra, A., Gomez-Sanchez, M. A., Rubenfire, M., Barbera, J. A., Channick, R. N., Naeije, R., Marini, C., Berman-Rosenzweig, E., Robbins, I. M., Girgis, R. E., Tapson, V. F., Delcroix, M., Kiely, D. G., Wodniecki, J., Schauer, J., Hoeper, M., Lim, S. T., Tack, S. J., Reuter, H., Carlsen, J., Lang, C. C., Roman, A., Benza, R. L., Williams, T. J., Corris, P. A., Zaba, J. P., Apro, D., Ghali, J. K., Badesch, D. B., Rich, S., Ross, D. J., Schulze-Neick, I., Martensson, G., Antonio Augusto Lopes, Andreassen, A. K., and Super Study Grp

169. Developing catalytic enantioselective fluorination

Author

Togni, A., Mezzetti, A., Barthazy, P., Becker, C., Devillers, I., Frantz, R., Lukas Hintermann, Perseghini, M., and Sanna, M.

Subjects
Ruthenium fluoro complexes, Chemistry, Titanium taddolato complexes, Asymmetric catalysis, Enantioselective fluorination, Enantioselective chlorination, General Medicine, General Chemistry, QD1-999
Abstract

The background that led to the development ofthe first catalytic and enantioselective carbon-fluorine bond-forming reaction is presented. Two different approaches, i.e. the use of nucleophilic and electrophilic fluorinating agents, respectively, have been pursued. Well-defined RU(II) 16-electron systems of the type [RuF(PP)2]+ (where PP is a chelating diphosphine), as well as analogous complexes containing tetradentate PNNP ligands, were found to catalyze the halogen exchange reaction of activated alkyl chlorides, bromides, and iodides in the presence of TIF as the fluorine source. Isolable crystalline [TiCl2 (TADDOLato)] complexes are efficient catalysts in the enantioselective fluorination of 2-substituted 1,3-dicarbonyl compounds with Selectfluor® (also called F-TEDA; 1-chloromethyl-4-fluoro-1,4-diazoniabicyclo[2.2.2]octane bis{tetrafluoroborate}). Levels of enantioselectivity up to 90% ee were obtained.

182. Contributors

Author

Aaron, Cynthia K., Abbott, Jean T., Abu-Laban, Riyad B., Adams, Bruce D., Adams, James G., Adams, Stephen L., Adirim, Terry A., Alagappan, Kumar, Amsterdam, James T., Anderegg, Christine, Anderson, Megan L., Anglin, Deirdre, Ankel, Felix, Arora, Sanjay, Aufderheide, Tom P., Ban, Kevin M., Baran, Emily, Bardsley, Christina E. Hantsch, Barkin, Adam Z., Barnosky, Andrew R., Barsan, William G., Becker, Bruce M., Bengiamin, Rimon N., Berg, Marc D., Berg, Robert A., Berkowitz, Carol D., Bernstein, Edward, Bernstein, Judith, Bessen, Howard A., Bhatia, Kriti, Bilden, Elisabeth F., Birnbaumer, Diane M., Biros, Michelle H., Bitterman, Robert A., Blackwell, Thomas H., Blum, Frederick C., Blumen, Ira J., Bocock, Jennifer M., Bolgiano, Edward B., Bontempo, Laura J., Brady, William J., Braithwaite, Sabina, Brown, Calvin A., III, Brown, James E., Brunette, Douglas D., Budhram, Gavin R., Bunney, E. Bradshaw, Burbulys, David, Burns, Michael J., Byyny, Richard L., Cahill, John D., Calder, Kirsten K., Cantor, Richard M., Caplen, Stuart M., Carlson, Andrea, Chan, Theodore C., Chen, Lei, Choi, Stephen B., Clark, Richard F., Clement, Philip A., Coates, Wendy C., Collier, Robert E., Collings, Jamie L., Colucciello, Stephen A., Colwell, Christopher B., Conway, Edward E., Jr., Cooke, Jeremy L., Cooper, Mary Ann, Cordle, Randolph J., Craig, Sandy A., Cranmer, Hilarie, Crocco, Todd J., Croskerry, Pat, Cwinn, A. Adam, Cydulka, Rita K., Danzl, Daniel F., Davitt, Ana M., Daya, Mohamud, Delaney, Kathleen A., Delbridge, Theodore R., Lorenzo, Robert A. De, Derlet, Robert W., Desai, Shoma, Dolcourt, Bram A., Duvivier, Evelyn H., Easter, Joshua S., Eckstein, Marc, Eisenhauer, Mary, Emery, Matt, Falk, Jay L., Feng, Sing-Yi, Fernández-Frackelton, Madonna, Fiechtl, James F., Finnell, John T., II, Fitch, Robert W., Foran, Mark, Gallagher, E. John, Garber, Boris, Gausche-Hill, Marianne, Gebhart, Mark E., Geiderman, Joel M., Gibbs, Michael A., Glass, Casey M., Goldberg, Richard, Gough, John E., Graff, Louis, IV, Gray, Richard O., Gross, Eric, Guisto, John A., Guss, David A., Gussow, Leon, Habal, Rania, Haile-Mariam, Tenagne, Hamilton, Glenn C., Hargarten, Stephen W., Harrigan, Richard A., Heegaard, William G., Heer, Jag S., Heilpern, Katherine L., Hemphill, Robin R., Henderson, Sean O., Hendrickson, Robert G., Henneman, Philip L., Hern, Jr., H. Gene, Ho, Kendall, Hockberger, Robert S., Hoffman, Robert S., Honigman, Benjamin, Horeczko, Timothy, Hostetler, Mark A., Houry, Debra E., Huff, J. Stephen, Hung, Oliver, Hutson, H. Range, Inaba, Alson S., Isenhour, Jennifer L., Iserson, Kenneth V., Jackimczyk, Kenneth, Jagoda, Andy, James, Thea L., Janz, Timothy G., Jones, Alan, Jones, James B., Jones, Jonathan S., Jouriles, Nicholas J., Kaji, Amy H., Kalbfleisch, Norman, Kao, Louise, Katz, Dan, Keadey, Matthew T., Kercher, Eugene E., Kiai, Kianusch, King, Kelly E., Kirelik, Susan, Klein, Eileen J., Kline, Jeffrey A., Knaut, Andrew L., Koenig, Kristi L., Kontrick, Amy V., Kornblau, Dina Halpern, Kosowsky, Joshua M., Kothari, Rashmi U., Krauss, Baruch, Kulig, Ken, Kwiatkowski, Thomas, Lavoie, Frank W., Lavonas, Eric J., Lee, Christopher C., Lee, David C., Lehrmann, Jill F., Lerner, E. Brooke, Levine, Michael D., Lewis, Roger J., Lin, Michelle, Ling, Louis J., Lipsky, Ari M., Losman, Eve D., Lowell, Mark J., Lowery, Douglas W., III, Ly, Binh T., Lyn, Everett T., Mahadevan, Malcolm, Mahoney, Brian D., Mailhot, Thomas, Mallon, William K., Maloney, Jr., Gerald E., Mandavia, Diku P., Manno, Mariann, Marco, Catherine A., Markovchick, Vincent, Martel, Marc L., Marx, John A., Mayersak, Ryanne J., Mazor, Suzan S., McCollough, Maureen, McKay, Mary Pat, McKenzie, L. Kendall, McKeown, Nathanael J., McManus, John, McMicken, David B., McQuillen, Kemedy K., Meislin, Harvey W., Melio, Frantz R., Meurer, William J., Mick, Nathan W., Miner, James R., Mitchell, Connie, Moore, Gregory P., Moran, Gregory J., Morrison, Laurie J., Muelleman, Robert L., Murray, Lindsay, Murphy, Michael F., Nadkarni, Vinay M., Nakamura, Yoko, Nelson, Lewis S., Neumar, Robert W., Newton, Edward J., Newton, Kim, Niemann, James T., Nowak, Richard M., O’Brien, John F., Olshaker, Jonathan S., Otten, Edward J., Oyama, Leslie C., Pallin, Daniel J., Paris, Paul M., Perina, Debra, Perron, Andrew D., Perry, Shawna J., Peterson, Michael A., Pfaff, James A., Pfeil, Sharon, Phillips, William James, Platt, Melissa, Polis, Michael Alan, Pollack, Charles V., Price, Timothy G., Purcell, Thomas B., Ramanujam, Prasanthi, Rao, Rama B., Raukar, Neha P., Rhee, James W., Richards, David B., Richards, John R., Roberts, David J., Rodenberg, Howard, Rodgers, Kevin G., Rothman, Richard E., Rubin, David H., Rund, Douglas A., Runyon, Michael S., Russi, Christopher S., Salhi, Bisan A., Santen, Sally A., Saveanu, Radu V., Scarfone, Richard J., Schmidt, Michael J., Schneider, Diana C., Schultz, Carl H., Schwartz, Richard B., Scott, Susan M., Seger, Donna L., Seiden, Jeffrey A., Seirafi, Jennifer, Sercombe, Clare T., Sexton, Joseph D., Shapiro, Marc J., Shapiro, Nathan I., Sharieff, Ghazala Q., Sharma, Rahul, Shearer, Peter, Shih, Richard D., Shoenberger, Jan M., Shockley, Lee W., Silbergleit, Robert, Simon, Barry C., Singer, Adam J., Singer, Jonathan I., Singh, Amardeep, Slaughter, Laura, Smith, Jeffrey Paul, Smock, William Spafford, Sokolove, Peter E., Soroff, Harry S., Squire, Benjamin, Stettler, Brian A., Stewart, Sara T., Stocker, David M., Stone, Susan, Strote, Jared, Swadron, Stuart P., Tadros, Allison, Taira, Breena R., Talan, David A., Tayal, Vivek S., Thomas, Stephen H., Tibbles, Carrie D., Tobias, Joshua J., Tokarski, Glenn F., Tomaszewski, Christian, Torbati, Sam S., Torrey, Susan P., Tran, T. Paul, Ugras-Rey, Sandra, Vakil, Monira, Vary, Marshall G., Velez, Larissa I., Vicario, Salvator, Vissers, Robert J., Walls, Ron M., Watson, Mark, Wax, Paul M., Wears, Robert L., Weber, Ellen J., West, Hugh H., Wheatley, Matthew A., White, Benjamin A., White, Suzanne R., Wiebe, Robert A., Wightman, John M., Williams, Saralyn R., Winter, Adria O., Wittler, Mary A., Wolfe, Jeannette M., Wolfson, Allan B., H. Woolfrey, Karen G., Woolfrey, Michael, Wright, Joshua L., Yang, Samuel, Yaron, Michael, Yealy, Donald M., Young, Amy, Young, Kelly D., Younger, John G., Zane, Richard, Zich, David K., Zimmer, Gary D., Zink, Brian J., Zull, David, and Zun, Leslie S.

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184. GIP Receptor Antagonism Eliminates Paradoxical Growth Hormone Secretion in Some Patients With Acromegaly.

Author

Jensen MH, Gasbjerg LS, Skov-Jeppesen K, Jacobsen JCB, Poulsen SS, Zhou C, Jakubauskaite R, Poulsen FR, Bonde C, Albarazi M, Halle B, Christiansen CB, Sanni SJ, Byberg S, Hoe B, Holst JJ, Dela F, Rasmussen AK, Knop FK, Arlien-Søborg MC, Melmed S, Jørgensen JOL, Andersen MS, Hartmann B, Klose MC, Feldt-Rasmussen U, Sparre-Ulrich AH, and Rosenkilde MM

Subjects
Humans, Male, Female, Middle Aged, Adult, Adenoma metabolism, Adenoma drug therapy, Adenoma pathology, Peptide Fragments metabolism, Aged, Acromegaly drug therapy, Acromegaly metabolism, Receptors, Gastrointestinal Hormone metabolism, Receptors, Gastrointestinal Hormone antagonists & inhibitors, Gastric Inhibitory Polypeptide metabolism, Human Growth Hormone metabolism, Glucose Tolerance Test, Growth Hormone-Secreting Pituitary Adenoma metabolism, Growth Hormone-Secreting Pituitary Adenoma drug therapy, Growth Hormone-Secreting Pituitary Adenoma pathology
Abstract

Context: About 30% of patients with active acromegaly experience paradoxically increased growth hormone (GH) secretion during the diagnostic oral glucose tolerance test (OGTT). Endogenous glucose-dependent insulinotropic polypeptide (GIP) is implicated in this paradoxical secretion., Objective: We used the GIP receptor (GIPR) antagonist GIP(3-30)NH2 to test the hypothesis that GIP mediates this paradoxical response when GIPR is abundantly expressed in somatotropinomas., Methods: A total of 25 treatment-naive patients with acromegaly were enrolled. Each patient underwent one OGTT during simultaneous placebo infusion and one OGTT during a GIP(3-30)NH2 infusion. Blood samples were drawn at baseline and regularly after infusions to measure GH. We assessed pituitary adenoma size by magnetic resonance imaging and GIPR expression by immunohistochemistry on resected somatotropinomas. For mechanistic confirmation, we applied in vitro and ex vivo approaches. The main outcome measure was the effect of GIP(3-30)NH2 on paradoxical GH secretion during OGTT as a measure of GIP involvement., Results: In 4 of 7 patients with paradoxical GH secretion, GIP(3-30)NH2 infusion completely abolished the paradoxical response (P = .0003). Somatotrophs were available from 3 of 4 of these patients, all showing abundant GIPR expression. Adenoma size did not differ between patients with and without paradoxical GH secretion., Conclusion: Of 25 patients with acromegaly, 7 had paradoxical GH secretion during OGTT, and pharmaceutical GIPR blockade abolished this secretion in 4. Corresponding somatotroph adenomas abundantly expressed GIPR, suggesting a therapeutic target in this subpopulation of patients. In vitro and ex vivo analyses confirmed the role of GIP and the effects of the antagonist., (© The Author(s) 2024. Published by Oxford University Press on behalf of the Endocrine Society.)

Published
2025
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185. Association of Phosphodiesterase-5 Inhibitor Treatment With Improved Survival in Pulmonary Hypertension Associated With COPD in the Pulmonary Vascular Research Institute GoDeep Meta-Registry.

Author

Tello K, Yogeswaran A, Majeed RW, Kiely DG, Lawrie A, Brittain E, Annis JS, Olschewski H, Kovacs G, Hassoun PM, Balasubramanian A, Konswa Z, Sweatt AJ, Zamanian RT, Wilkins MR, Howard L, Arvanitaki A, Giannakoulas G, Cajigas HR, Frantz R, Williams PG, Frauendorf M, Marquardt K, Antoine T, Fuenderich M, Richter M, Grimminger F, Ghofrani HA, Wilhelm J, and Seeger W

Subjects
Humans, Male, Female, Middle Aged, Aged, Vascular Resistance, Survival Rate, Pulmonary Disease, Chronic Obstructive drug therapy, Pulmonary Disease, Chronic Obstructive complications, Pulmonary Disease, Chronic Obstructive mortality, Pulmonary Disease, Chronic Obstructive physiopathology, Hypertension, Pulmonary drug therapy, Hypertension, Pulmonary mortality, Hypertension, Pulmonary etiology, Hypertension, Pulmonary physiopathology, Phosphodiesterase 5 Inhibitors therapeutic use, Registries
Abstract

Background: Patients with COPD frequently demonstrate pulmonary hypertension (PH). Severe PH in patients with COPD, identified by pulmonary vascular resistance (PVR) of > 5 Wood units (WU), is closely linked to impaired transplant-free survival. The impact of PH-targeting pharmacotherapy in this context remains unclear., Research Question: Is PH-targeted therapy associated with improved transplant-free survival in patients with COPD and PH?, Study Design and Methods: This study included Pulmonary Vascular Research Institute GoDeep meta-registry patients with COPD and PH and available right heart catheterization at diagnosis. We investigated PH-targeted therapy prevalence and its association with transplant-free survival using diverse statistical methods, including Cox regression and subgroup analyses based on PH severity, comorbidities, and pulmonary function test results. Immortal time bias was addressed through a landmark approach., Results: As of December 2023, the GoDeep meta-registry included 26,981 patients (28% in PH group 1, 13% in PH group 2, 12% in PH group 3, 10% in PH group 4, 2% in PH group 5, 26% undefined, and 9% control participants). Of these, 836 patients had a diagnosis of COPD with PH and were included in this analysis, with median age of 66 years (interquartile range [IQR], 59-73 years), FEV 1 of 51% predicted (IQR, 34%-69% predicted), mPAP of 35 mm Hg (IQR, 28-44 mm Hg), PVR of 5 WU (IQR, 4-8 WU), cardiac index of 2.5 L/min/m 2 (IQR, 2.0-2.9 L/min/m 2 ), and mostly World Health Organization functional class III were included. Five-year transplant-free survival was 42%, significantly worse than in group 1 PH. A multivariable Cox proportional hazards model identified PVR, but not FEV 1 , as a major predictor of outcome. Four hundred eighteen patients (50%) received phosphodiesterase-5 inhibitor (PDE5i) therapy, which was associated with significantly reduced mortality: hazard ratio of 0.65 (IQR, 0.57-0.75) for the entire cohort of patients with COPD and PH and of 0.83 (IQR, 0.74-0.94) when performing landmark analysis. This PDE5i effect was reproduced robustly when performing subgroup analyses for patients with moderate to severe PH, various comorbidities, and supplemental oxygen requirement and when assessing the impact of unobserved confounders., Interpretation: Patients with COPD and PH exhibit poor transplant-free survival, with PVR being a predictor of mortality. In this meta-registry, PDE5i therapy was associated with a significant reduction in mortality across all tested models., Competing Interests: Financial/Nonfinancial Disclosures The authors have reported to CHEST the following: K. T. has received personal fees from Bayer, AstraZeneca, and Gossamer. A. Y. has received personal fees from MSD and support for scientific meetings from AOP. D. G. K. reports support from the Sheffield Biomedical Research Centre and consulting fees and other payments from Jansen Pharmaceuticals, Ferrer, Altavant, MSD, and United therapeutics. H. O. reports grants or contracts from Actelion, Bayer, Boehringer-Ingelheim, Janssen, MSD, IQVIA, and Pfizer; consulting fees from Bayer and IQVIA; speaker fees from Actelion, Bayer, Boehringer-Ingelheim, MSD, and Pfizer; support for scientific meetings from Astra Zeneca, Boehringer-Ingelheim, Menarini, and MSD; and participation on data safety board or advisory board for Bayer and IQVIA. G. K. reports consulting and speaker fees from Boehringer-Ingelheim, Janssen, MSD, Astra Zeneca, Chiesi, AOP, and Ferrer and support for scientific meetings from AOP, Vitalaire, MSD, and Boehringer-Ingelheim. P. M. H. reports personal fees from Merck Co. M. R. W. reports personal fees from MorphogenIX, Janssen, Chiesi, and Aerami; grants from British Heart Foundation and NIHR; and personal fees from MSD, Benevolent AI, and Tiakis Biotech outside the submitted work. L. H. reports personal fees and nonfinancial support from Janssen and personal fees from MSD, Gossamer, and Altavant. M. R. has received support from Janssen Pharmaceutica and Bayer Pharma AG, and speaker fees from Janssen Pharmaceutica and OMT. H.-A. G. has received fees from Actelion, AstraZeneca, Bayer, GSK, Janssen-Cilag, Lilly, Novartis, OMT, Pfizer, and United Therapeutics. W. S. has received consultancy fees from United Therapeutics, Tiakis Biotech AG, Liquidia, Pieris Pharmaceuticals, Abivax, Pfizer, and Medspray BV. None declared (R. W. M., A. L., E. B., J. S. A., A. B., Z. K., A. J. S., R. T. Z., A. A., G. G., H. R. C., R. F., P. G. W., M. Frauendorf, K. M., T. A., M. Feunerich, F. G., J. W.)., (Copyright © 2024. Published by Elsevier Inc.)

Published
2025
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186. The risk of venous thromboembolism in adult patients with diffuse glioma: a nationwide population-based study.

Author

Hovman FR, Poulsen FR, Hansen S, and Dahlrot RH

Subjects
Humans, Male, Female, Middle Aged, Adult, Denmark epidemiology, Incidence, Risk Factors, Aged, Registries statistics & numerical data, Young Adult, Neoplasm Grading, Venous Thromboembolism epidemiology, Venous Thromboembolism etiology, Glioma complications, Glioma epidemiology, Brain Neoplasms epidemiology, Brain Neoplasms complications
Abstract

Background and Purpose: Venous thromboembolism (VTE) is a cause of increased morbidity and risk of death. Studies report VTE in up to 30% of glioma patients but the results vary. The VTE risk is relevant when evaluating prophylaxis to avoid unnecessary bleeding or overdiagnosis. This study examines the VTE incidence in patients with glioma WHO grade 2-4, and when VTE occurred, risk factors, and overall survival (OS) for patients with WHO grade 4., Materials and Methods: In total 3,630 patients with WHO grade 2 (n = 230), grade 3 (n = 317), and grade 4 (n = 3,083) gliomas from 2010 to 2018 were identified using the Danish Neuro-Oncology Registry. VTE diagnoses and time of death were obtained from Statistics Denmark., Results and Interpretation: The VTE incidence was 5.2, 6.3, and 6.8% in patients with WHO grade 2, 3, and 4 gliomas, respectively. The VTE incidence rate was highest during the first 3 months after the diagnosis with 53 events. Increasing age (HR 1.03, 95%CI 1.01-1.04), male sex (HR 1.47, 95%CI 1.09-1.99), poor performance status (HR 1.57, 95%CI 1.10-2.25), and post-operative long-course radiochemotherapy (HR 2.10, 95%CI 1.19-3.72) were predictors of VTE in patients with glioma WHO grade 4. There was no difference in OS comparing patients having VTE to those without (p = 0.068). In conclusion, patients with glioma WHO grade 2-4 were at high risk of VTE, especially the first 3 months after diagnosis. Increasing age, male sex, poor performance status, and long-course radiochemotherapy were associated with increased risk of VTE in patients with glioma WHO grade 4.

Published
2024
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187. Risk stratification and treatment goals in pulmonary arterial hypertension.

Author

Dardi F, Boucly A, Benza R, Frantz R, Mercurio V, Olschewski H, Rådegran G, Rubin LJ, and Hoeper MM

Subjects
Humans, Risk Assessment, Prognosis, Biomarkers blood, Hypertension, Pulmonary therapy, Hemodynamics, Natriuretic Peptides blood, Severity of Illness Index, Walk Test, Pulmonary Arterial Hypertension physiopathology
Abstract

Risk stratification has gained an increasing role in predicting outcomes and guiding the treatment of patients with pulmonary arterial hypertension (PAH). The most predictive prognostic factors are three noninvasive parameters (World Health Organization functional class, 6-min walk distance and natriuretic peptides) that are included in all currently validated risk stratification tools. However, suffering from limitations mainly related to reduced specificity of PAH severity, these variables may not always be adequate in isolation for guiding individualised treatment decisions. Moreover, with effective combination treatment regimens and emerging PAH therapies, markers associated with pulmonary vascular remodelling are expected to become of increasing relevance in guiding the treatment of patients with PAH. While reaching a low mortality risk, assessed with a validated risk tool, remains an important treatment goal, preliminary data suggest that invasive haemodynamics and cardiac imaging may add incremental value in guiding treatment decisions., Competing Interests: Conflict of interest: F. Dardi reports consultancy fees from Janssen and Chiesi Farmaceutici, and payment or honoraria for lectures, presentations, manuscript writing or educational events from Janssen. A. Boucly reports grants from Acceleron, Janssen and MSD, payment or honoraria for lectures, presentations, manuscript writing or educational events from Janssen, Merck, AOP Orphan, Ferrer and AstraZeneca, and support for attending meetings from Janssen, MSD, Ferrer and AOP Orphan. R. Benza reports consultancy fees from Cereno, Gossamer and United Therapeutics, and participation on a data safety monitoring board or advisory board with Altavant. R. Frantz reports grants from NHLBI and Gossamer Bio, royalties or licences from UpToDate, consultancy fees from Gossamer Bio, Insmed, Merck and Liquidia, participation on a data safety monitoring board or advisory board with Aerovate Pharmaceuticals, leadership role with Pulmonary Hypertension Association Scientific Leadership Council, and stock (or stock options) with Merck. V. Mercurio reports consultancy fees from MSD, payment or honoraria for lectures, presentations, manuscript writing or educational events from Janssen, and support for attending meetings from Janssen and MSD. H. Olschewski reports consultancy fees from Actelion, AstraZeneca, Bayer, Boehringer, Janssen, MSD, Chiesi, GSK, Inventiva, Ferrer, Menarini and Sanofi, payment or honoraria for lectures, presentations, manuscript writing or educational events from Springer, Medupdate and Mondial, support for attending meetings from Boehringer, Menarini and MSD, participation on a data safety monitoring board or advisory board with Aerovate, Bayer, Pfizer and IQVIA, receipt of equipment, materials, drugs, medical writing, gifts or other services from Boehringer, and the following financial (or non-financial) interests: Deputy Director, Ludwig Boltzmann Institute for Lung Vascular Research, Graz. G. Rådegran reports grants from Nordic Infucare, payment or honoraria for lectures, presentations, manuscript writing or educational events from Janssen, MSD, Nodic Infucare and Orpha Care/AOP Health, and participation on a data safety monitoring board or advisory board with Janssen, MSD and Orpha Care/AOP Health. L.J. Rubin reports consultancy fees from Gossamer and SoniVie, payment for expert testimony from Sandoz, and is a member of the Organizing and Founders Committees, WSPH. M.M. Hoeper reports consultancy fees from Acceleron, Actelion, AOP Health, Bayer, Ferrer, Gossamer Bio, Janssen, Keros and MSD, and payment or honoraria for lectures, presentations, manuscript writing or educational events from Actelion, AOP Health, Bayer, Ferrer, Janssen and MSD., (Copyright ©The authors 2024.)

Published
2024
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188. Brain targeting for focused ultrasound essential tremor ablation: proceedings from the 2023 Focused Ultrasound Foundation workshop.

Author

Chua MMJ, LeBlang S, Powlovich L, Gilbertson T, Krishna V, Guttmann CRG, Eames MDC, Poulsen FR, and Cosgrove GR

Subjects
Humans, High-Intensity Focused Ultrasound Ablation methods, Brain surgery, Brain diagnostic imaging, Magnetic Resonance Imaging methods, Essential Tremor surgery, Essential Tremor diagnostic imaging, Essential Tremor therapy, Thalamus surgery, Thalamus diagnostic imaging
Abstract

Essential tremor (ET) is the most common movement disorder globally and has negative impacts on quality of life. While medical treatments exist, approximately 50% of patients have tremor that is refractory to medication or experience intolerable medication side effects. Magnetic resonance-guided focused ultrasound (MRgFUS) thalamotomy is an option for these patients and while incisionless, it is still invasive, although less so than other surgical treatments such as deep brain stimulation and radiofrequency thalamotomy. Despite MRgFUS being FDA-approved since 2016, there is still no current consensus on the best approaches for targeting, imaging, and outcome measurement. A 2-day workshop held by the Focused Ultrasound Foundation in September of 2023 convened experts and critical stakeholders in the field to share their knowledge and experiences. The goals of the workshop were to determine the optimal target location within the thalamus and compare best practices for localizing the target and tracking patient outcomes. This paper summarizes the current landscape, important questions, and discussions that will help direct future treatments to improve patient care and outcomes.

Published
2024
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189. Comparison of Contemporary Risk Scores in All Groups of Pulmonary Hypertension: A Pulmonary Vascular Research Institute GoDeep Meta-Registry Analysis.

Author

Yogeswaran A, Gall H, Fünderich M, Wilkins MR, Howard L, Kiely DG, Lawrie A, Hassoun PM, Sirenklo Y, Torbas O, Sweatt AJ, Zamanian RT, Williams PG, Frauendorf M, Arvanitaki A, Giannakoulas G, Saleh K, Sabbour H, Cajigas HR, Frantz R, Al Ghouleh I, Chan SY, Brittain E, Annis JS, Pepe A, Ghio S, Orfanos S, Anthi A, Majeed RW, Wilhelm J, Ghofrani HA, Richter MJ, Grimminger F, Sahay S, Tello K, and Seeger W

Subjects
Humans, Prognosis, Risk Assessment methods, Hypertension, Pulmonary epidemiology, Hypertension, Pulmonary physiopathology, Registries statistics & numerical data
Abstract

Background: Pulmonary hypertension (PH) is a heterogeneous disease with a poor prognosis. Accurate risk stratification is essential for guiding treatment decisions in pulmonary arterial hypertension (PAH). Although various risk models have been developed for PAH, their comparative prognostic potential requires further exploration. Additionally, the applicability of risk scores in PH groups beyond group 1 remains to be investigated., Research Question: Are risk scores originally developed for PAH predictive in PH groups 1 through 4?, Study Design and Methods: We conducted a comprehensive analysis of outcomes among patients with incident PH enrolled in the multicenter worldwide Pulmonary Vascular Research Institute GoDeep meta-registry. Analyses were performed across PH groups 1 through 4 and further subgroups to evaluate the predictive value of PAH risk scores, including the Registry to Evaluate Early and Long-Term PAH Disease Mangement (REVEAL) Lite 2, REVEAL 2.0, European Society of Cardiology/European Respiratory Society 2022, Comparative, Prospective Registry of Newly Initiated Therapies for Pulmonary Hypertension (COMPERA) 3-strata, and COMPERA 4-strata., Results: Eight thousand five hundred sixty-five patients were included in the study, of whom 3,537 patients were assigned to group 1 PH, whereas 1,807 patients, 1,635 patients, and 1,586 patients were assigned to group 2 PH, group 3 PH, and group 4 PH, respectively. Pulmonary hemodynamics were impaired with median mean pulmonary arterial pressure of 42 mm Hg (interquartile range, 33-52 mm Hg) and pulmonary vascular resistance of 7 Wood units (WU) (interquartile range, 4-11 WU). All risk scores were prognostic in the entire PH population and in each of the PH groups 1 through 4. The REVEAL scores, when used as continuous prediction models, demonstrated the highest statistical prognostic power and granularity; the COMPERA 4-strata risk score provided subdifferentiation of the intermediate-risk group. Similar results were obtained when separately analyzing various subgroups (PH subgroups 1.1, 1.4.1, and 1.4.4; PH subgroups 3.1 and 3.2; group 2 with isolated postcapillary PH vs combined precapillary and postcapillary PH; patients of all groups with concomitant cardiac comorbidities; and severe [> 5 WU] vs nonsevere PH)., Interpretation: This comprehensive study with real-world data from 15 PH centers showed that PAH-designed risk scores possess predictive power in a large PH cohort, whether considered as common to the group or calculated separately for each PH group (1-4) and various subgroups., Trial Registry: ClinicalTrials.gov; No.: NCT05329714; URL: www., Clinicaltrials: gov., Competing Interests: Financial/Nonfinancial Disclosures The authors have reported to CHEST the following: A. Y. has received personal fees from MSD. H. G. has received personal fees from Actelion, AstraZeneca, Bayer, BMS, GossamerBio, GSK, Janssen-Cilag, Lilly, MSD, Novartis, OMT, Pfizer, and United Therapeutics. M. R. W. reports personal fees from MorphogenIX, Janssen, Chiesi, and Aerami; grants from British Heart Foundation and NIHR; and personal fees from MSD, Benevolent AI, and Tiakis Biotech, outside the submitted work. L. H. reports personal fees and nonfinancial support from Janssen and personal fees from MSD, Gossamer, and Altavant. D. G. K. reports support for the present manuscript from the Sheffield Biomedical Research Centre and consulting fees and other payments from Jansen Pharmaceuticals, Ferrer, Altavant, MSD, and United therapeutics. P. M. H. reports personal fees from Merck Co. S. Y. C. reports personal fees from Janssen, Bayer, Pfizer, United Therapeutics, and Acceleron Pharma and is a director, officer, and shareholder of Synhale Therapeutics. S. O. reports personal fees from MSD, Janssen, and Gallenica-Ferrer. H. A. G. has received fees from Actelion, AstraZeneca, Bayer, GSK, Janssen-Cilag, Lilly, Novartis, OMT, Pfizer, and United Therapeutics. M. J. R. has received support from Janssen Pharmaceutica and Bayer Pharma AG and speaker fees from Janssen Pharmaceutica and OMT. S. S. reports personal fees from Gossamer Bio, Merck, Keros, Janssen, United Therapeutics, and Liquidia. K. T. has received personal fees from Bayer, AstraZeneca, and Gossamer. W. S. has received consultancy fees from United Therapeutics, Tiakis Biotech AG, Liquidia, Pieris Pharmaceuticals, Abivax, Pfitzer, and Medspray BV. None declared (M. Fünderich, A.L., Y. S., O. T., A. J. S., R. T. Z., P. G. W., M. Frauendorf, A. Arvanitaki, G. G., K. S., H. R. C., R. F., I. A. G., E. B., J. S. A., A. P., S. G., A. Anthi, R. W. M., J. W., F. G.), (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published
2024
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190. Prognostic factors to predict postoperative survival in patients with recurrent glioblastoma.

Author

Hansen ST, Jacobsen KS, Kofoed MS, Petersen JK, Boldt HB, Dahlrot RH, Schulz MK, and Poulsen FR

Abstract

Background: There are no generally accepted criteria for selecting patients with recurrent glioblastoma for surgery. This retrospective study in a Danish population-based cohort aimed to identify prognostic factors affecting postoperative survival after repeated surgery for recurrent glioblastoma and to test if the preoperative New Scale for Recurrent Glioblastoma Surgery (NSGS) developed by Park CK et al could assist in the selection of patients for repeat glioblastoma surgery., Methods: Clinical data from 66 patients with recurrent glioblastoma and repeated surgery were analyzed. Kaplan-Meier plots were produced to illustrate survival in each of the three NSGS prognostic groups, and Cox proportional hazard regression was used to identify prognostic variables. Multivariable analysis was used to identify differences in survival in the three prognostic groups., Results: Six variables significantly affected postoperative survival: preoperative Karnofsky Performance Status (KPS) < 70 ( p  = 0.002), decreased KPS after second surgery ( p  = 0.012), ependymal involvement ( p  = 0.002), tumor volume ≧ 50 cm 3  ( p  = 0.021), age ( p  = 0.033) and Ki-67 ( p  = 0.005). Retrospective application of the criteria previously published by Park CK et al showed that median postoperative survival for the three prognostic groups was 390 days (0 points), 279 days (1 point), and 80 days (2 points), respectively., Conclusion: Several prognostic variables to predict postoperative survival in patients with recurrent glioblastoma were identified and should be considered when selecting patient for repeat surgery. The NSGS scoring system was useful as there were significant differences in postoperative survival between its three prognostic groups., Competing Interests: The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (© 2024 The Authors.)

Published
2024
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191. Frequency of acute vasodilator response (AVR) in incident and prevalent patients with pulmonary arterial hypertension: Results from the pulmonary vascular disease phenomics study.

Author

Naranjo M, Rosenzweig EB, Hemnes AR, Jacob M, Desai A, Hill NS, Larive AB, Finet JE, Leopold J, Horn E, Frantz R, Rischard F, Erzurum S, Beck G, Mathai SC, and Hassoun PM

Abstract

The prevalence of acute vasodilator response (AVR) to inhaled nitric oxide (iNO) during right heart catheterization (RHC) is 12% in idiopathic pulmonary arterial hypertension (IPAH). AVR, however, is reportedly lower in other disease-associated pulmonary arterial hypertension (PAH), such as connective tissue disease (CTD). The prevalence of AVR in patients on PAH therapy (prevalent cases) is unknown. We sought to determine AVR prevalence in Group 1 PH in the PVDOMICS cohort of incident and prevalent patients undergoing RHC. AVR was measured in response to 100% O 2 and O 2 plus iNO, with positivity defined as (1) decrease in mean pulmonary artery pressure (mPAP) by ≥10 mmHg to a value ≤40 mmHg, with no change or an increase in cardiac output (definition 1); or (2) decrease in mPAP by ≥12% and pulmonary vascular resistance by ≥30% (definition 2). AVR rates and cumulative survival were compared between incident and prevalent patients. In 338 mainly prevalent (86%) patients, positive AVR to O 2 -only was <2%, and 5.1% to 16.9%, based on definition 1 and 2 criteria, respectively; following O 2  + iNO. IPAH AVR prevalence (4.1%-18.7%) was similar to prior reports. AVR positivity was 7.7% to 15.4% in mostly CTD-PAH prevalent cases, and 2.6% to 11.8% in other PAH groups. Survival was 89% in AVR responders versus 77% in nonresponders from PAH diagnosis, and 91% versus 86% from PVDOMICS enrollment (log-rank test p  = 0.04 and p  = 0.05, respectively). In conclusion, AVR in IPAH patients is similar to prior studies. AVR in non-IPAH patients was higher than previously reported. The relationship between PAH therapy, AVR response, and survival warrants further investigation., Competing Interests: The authors declare no conflict of interest., (© 2023 The Authors. Pulmonary Circulation published by John Wiley & Sons Ltd on behalf of Pulmonary Vascular Research Institute.)

Published
2023
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192. A Single Residue within the MCR-1 Protein Confers Anticipatory Resilience.

Author

Frantz R, Gwozdzinski K, Gisch N, Doijad SP, Hudel M, Wille M, Abu Mraheil M, Schwudke D, Imirzalioglu C, Falgenhauer L, Ehrmann M, and Chakraborty T

Subjects
Lipid A, Anti-Bacterial Agents pharmacology, Escherichia coli, Plasmids, Peptide Hydrolases pharmacology, Drug Resistance, Bacterial genetics, Microbial Sensitivity Tests, Colistin pharmacology, Escherichia coli Proteins genetics, Escherichia coli Proteins metabolism
Abstract

The envelope stress response (ESR) of Gram-negative enteric bacteria senses fluctuations in nutrient availability and environmental changes to avert damage and promote survival. It has a protective role toward antimicrobials, but direct interactions between ESR components and antibiotic resistance genes have not been demonstrated. Here, we report interactions between a central regulator of ESR viz. , the two-component signal transduction system CpxRA ( c onjugative p ilus e x pression), and the recently described mobile colistin resistance protein (MCR-1). Purified MCR-1 is specifically cleaved within its highly conserved periplasmic bridge element, which links its N-terminal transmembrane domain with the C-terminal active-site periplasmic domain, by the CpxRA-regulated serine endoprotease DegP. Recombinant strains harboring cleavage site mutations in MCR-1 are either protease resistant or degradation susceptible, with widely differing consequences for colistin resistance. Transfer of the gene encoding a degradation-susceptible mutant to strains that lack either DegP or its regulator CpxRA restores expression and colistin resistance. MCR-1 production in Escherichia coli imposes growth restriction in strains lacking either DegP or CpxRA, effects that are reversed by transactive expression of DegP. Excipient allosteric activation of the DegP protease specifically inhibits growth of isolates carrying mcr-1 plasmids. As CpxRA directly senses acidification, growth of strains at moderately low pH dramatically increases both MCR-1-dependent phosphoethanolamine (PEA) modification of lipid A and colistin resistance levels. Strains expressing MCR-1 are also more resistant to antimicrobial peptides and bile acids. Thus, a single residue external to its active site induces ESR activity to confer resilience in MCR-1-expressing strains to commonly encountered environmental stimuli, such as changes in acidity and antimicrobial peptides. Targeted activation of the nonessential protease DegP can lead to the elimination of transferable colistin resistance in Gram-negative bacteria. IMPORTANCE The global presence of transferable mcr genes in a wide range of Gram-negative bacteria from clinical, veterinary, food, and aquaculture environments is disconcerting. Its success as a transmissible resistance factor remains enigmatic, because its expression imposes fitness costs and imparts only moderate levels of colistin resistance. Here, we show that MCR-1 triggers regulatory components of the envelope stress response, a system that senses fluctuations in nutrient availability and environmental changes, to promote bacterial survival in low pH environments. We identify a single residue within a highly conserved structural element of mcr-1 distal to its catalytic site that modulates resistance activity and triggers the ESR. Using mutational analysis, quantitative lipid A profiling and biochemical assays, we determined that growth in low pH environments dramatically increases colistin resistance levels and promotes resistance to bile acids and antimicrobial peptides. We exploited these findings to develop a targeted approach that eliminates mcr-1 and its plasmid carriers., Competing Interests: The authors declare no conflict of interest.

Published
2023
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193. The heart of the matter: Right heart imaging indicators for treatment escalation in pulmonary arterial hypertension.

Author

Forfia P, Benza R, D'Alto M, De Marco T, Elwing JM, Frantz R, Haddad F, Oudiz R, Preston IR, Rosenkranz S, Ryan J, Schilz R, Shlobin OA, Vachiery JL, Vizza CD, Vonk Noordegraaf A, Sketch MR, Broderick M, and McLaughlin V

Abstract

Right heart (RH) structure and function are major determinants of symptoms and prognosis in pulmonary arterial hypertension (PAH). RH imaging provides detailed information, but evidence and guidelines on the use of RH imaging in treatment decisions are limited. We conducted a Delphi study to gather expert opinion on the role of RH imaging in decision-making for treatment escalation in PAH. A panel of 17 physicians with expertise in PAH and RH imaging used three surveys in a modified Delphi process to reach consensus on the role of RH imaging in PAH. Survey 1 used open-ended questions to gather information. Survey 2 contained Likert scale and other questions intended to identify consensus on topics identified in Survey 1. Survey 3 contained Likert scale questions derived from Survey 2 and summary information on the results of Survey 2. The Delphi panel reached consensus that RH imaging is likely to improve the current risk stratification algorithms and help differentiate risk levels in patients at intermediate risk. Tricuspid annular plane systolic excursion, right ventricular fractional area change, right atrial area, tricuspid regurgitation, inferior venae cavae diameter, and pericardial effusion should be part of routine echocardiography in PAH. Cardiac magnetic resonance imaging is valuable but limited by cost and access. A pattern of abnormal RH imaging results should prompt consideration of hemodynamic evaluation and possible treatment escalation. RH imaging is an important tool for decisions about treatment escalation in PAH, but systematically collected evidence is needed to clarify its role., Competing Interests: Paul Forfia has served on a speaker's bureau and consulted for Bayer, Janssen, and United Therapeutics. Raymond Benza has received consulting fees from Bayer, Janssen, United Therapeutics, Acceleron, CERENO, Abbott, and Gossamer; and advisory board fees from Acceleron. Michele D'Alto has received consulting fees from Janssen, MSD, Dompè, Ferrer, and AOP. Teresa De Marco has received research funding from Acceleron; and has served as a consultant for Action/Janssen, United Therapeutics, BIAL, Merck, NXT, Aerovate, and Pulnovo. Jean M. Elwing has served as a consultant for United Therapeutics, Altavant, Aerovate, Bayer, Gossamer Bio, Acceleron, Janssen, Liquid, and Insmed; and has participated in clinical research funded by Janssen, United Therapeutics, Liquidia, Phase Bio, Gossamer Bio, Bayer, Acceleron, Altavant, and Aerovate. Robert Frantz has received consulting fees from Altavant, Gossamer Bio, Insmed, Liquidia, ShouTi, and Tenax; serves on DSMB for IQVIA; and has received research grants from Bayer and United Therapeutics. Francois Haddad has received research funding from Janssen. Ronald Oudiz has received research funding, advisory board honoraria, and speaker fees from United Therapeutics. Ioana R. Preston has received research funding from Acceleron/Merck, Janssen, United Therapeutics, and PhaseBio; and consulting fees from Acceleron/Merck, Janssen, United Therapeutics, Aerovate, Gossamer Bio, and Respira. Stephan Rosenkranz has received fees for lectures and/or consultations from Abbott, Acceleron, Actelion, Aerovate, Altavant, AOP Orphan, AstraZeneca, Bayer, Boehringer Ingelheim, Edwards, Ferrer, Gossamer, Janssen, MSD, United Therapeutics, and Vifor; and his institution has received research grants from Actelion, AstraZeneca, Bayer, and Janssen. John Ryan has received consulting fees and payment or honoraria from lectures, presentations, speakers' bureaus, manuscript writing, or education events from Bayer, Merck, United Therapeutics, Kiniksa, and Janssen PH. Robert Schilz has received research funding from Acceleron/Merck, United Therapeutics, Respira, and Bellerophon; consulting fees from Janssen, United Therapeutics, and Acceleron; and currently serves on speakers' bureaus for Bayer, Janssen, and United Therapeutics. Oksana A. Shlobin has received consulting fees from United Therapeutics and Janssen; has received honoraria from Medscape, Total CME, and Bayer; and has participated in a Data Safety Monitoring Board or Advisory Board for Janssen and Altavant. Jean‐Luc Vachiery has received consulting fees from Acceleron, Actelion Pharmaceuticals (now Janssen), Altavant, Bayer HealthCare, Boehringer Ingelheim, GlaxoSmithKline, Gossamer Bio, MSD, Novartis, and Shouti. Carmine Dario Vizza has received consulting fees from Acceleron, Janssen, Altavant, Bayer HealthCare, Ferrer, GlaxoSmithKline, Gossamer Bio, and MSD. Anton Vonk Noordegraaf has served as a member of the scientific advisory board of Morphogen‐X, Ferrer, Gosamer Bio, and Johnson & Johnson. The institute of Anton Vonk Noordegraaf has received consulting fees from a speakers' bureau for Johnson & Johnson, MSD, Actelion, Bayer, and Ferrer. Margaret R. Sketch and Meredith Broderick are employees and shareholders of United Therapeutics Corporation. Vallerie McLaughlin has received research funding from Acceleron, Janssen, Sonovie, and United Therapeutics; and consulting fees from Acceleron, Aerovate, Altavant, Bayer, Caremark LLC, CiVi Biopharma Inc., Corvista, Gossamer Bio, Janssen, Merck, and United Therapeutics., (© 2023 The Authors. Pulmonary Circulation published by John Wiley & Sons Ltd on behalf of Pulmonary Vascular Research Institute.)

Published
2023
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194. Resolving colistin resistance and heteroresistance in Enterobacter species.

Author

Doijad SP, Gisch N, Frantz R, Kumbhar BV, Falgenhauer J, Imirzalioglu C, Falgenhauer L, Mischnik A, Rupp J, Behnke M, Buhl M, Eisenbeis S, Gastmeier P, Gölz H, Häcker GA, Käding N, Kern WV, Kola A, Kramme E, Peter S, Rohde AM, Seifert H, Tacconelli E, Vehreschild MJGT, Walker SV, Zweigner J, Schwudke D, and Chakraborty T

Subjects
Bacterial Proteins metabolism, Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents therapeutic use, Enterobacter genetics, Drug Resistance, Bacterial genetics, Microbial Sensitivity Tests, Colistin pharmacology, Colistin therapeutic use, Lipid A chemistry, Lipid A pharmacology
Abstract

Species within the Enterobacter cloacae complex (ECC) include globally important nosocomial pathogens. A three-year study of ECC in Germany identified Enterobacter xiangfangensis as the most common species (65.5%) detected, a result replicated by examining a global pool of 3246 isolates. Antibiotic resistance profiling revealed widespread resistance and heteroresistance to the antibiotic colistin and detected the mobile colistin resistance (mcr)-9 gene in 19.2% of all isolates. We show that resistance and heteroresistance properties depend on the chromosomal arnBCADTEF gene cassette whose products catalyze transfer of L-Ara4N to lipid A. Using comparative genomics, mutational analysis, and quantitative lipid A profiling we demonstrate that intrinsic lipid A modification levels are genospecies-dependent and governed by allelic variations in phoPQ and mgrB, that encode a two-component sensor-activator system and specific inhibitor peptide. By generating phoPQ chimeras and combining them with mgrB alleles, we show that interactions at the pH-sensing interface of the sensory histidine kinase phoQ dictate arnBCADTEF expression levels. To minimize therapeutic failures, we developed an assay that accurately detects colistin resistance levels for any ECC isolate., (© 2023. The Author(s).)

Published
2023
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195. SecA2 Associates with Translating Ribosomes and Contributes to the Secretion of Potent IFN-β Inducing RNAs.

Author

Teubner L, Frantz R, La Pietra L, Hudel M, Bazant J, Lochnit G, Eismann L, Kramer G, Chakraborty T, and Abu Mraheil M

Subjects
Humans, Adenosine Triphosphatases genetics, Adenosine Triphosphatases metabolism, Bacterial Proteins metabolism, RNA metabolism, Membrane Transport Proteins metabolism, Listeria monocytogenes
Abstract

Protein secretion plays a central role in modulating interactions of the human pathogen Listeria monocytogenes with its environment. Recently, secretion of RNA has emerged as an important strategy used by the pathogen to manipulate the host cell response to its advantage. In general, the Sec-dependent translocation pathway is a major route for protein secretion in L. monocytogenes , but mechanistic insights into the secretion of RNA by these pathways are lacking. Apart from the classical SecA1 secretion pathway, L. monocytogenes also encodes for a SecA paralogue (SecA2) which targets the export of a specific subset of proteins, some of which are involved in virulence. Here, we demonstrated that SecA2 co-sediments with translating ribosomes and provided evidence that it associates with a subset of secreted small non-coding RNAs (sRNAs) that induce high levels of IFN-β response in host cells. We found that enolase, which is translocated by a SecA2-dependent mechanism, binds to several sRNAs, suggesting a pathway by which sRNAs are targeted to the supernatant of L. monocytogenes .

Published
2022
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196. Tumors of the central nervous system among women treated with fertility drugs: a population-based cohort study.

Author

Frandsen CLB, Jensen A, Poulsen FR, Møller M, Lindquist S, Albieri V, Nøhr B, and Kjær SK

Subjects
Cohort Studies, Denmark epidemiology, Female, Humans, Risk Factors, Central Nervous System Neoplasms drug therapy, Central Nervous System Neoplasms epidemiology, Fertility Agents therapeutic use, Infertility, Female drug therapy, Infertility, Female epidemiology, Meningeal Neoplasms, Meningioma
Abstract

Purpose: To investigate the association between fertility drugs and tumors of the central nervous system (CNS)., Methods: This cohort study was based on The Danish Infertility Cohort and included 148,016 infertile women living in Denmark (1995-2017). The study cohort was linked to national registers to obtain information on use of specific fertility drugs, cancer diagnoses, covariates, emigration, and vital status. Cox proportional hazard regression models were used to calculate hazard ratios (HRs) and 95% confidence intervals (CIs) for all CNS tumors and separately for gliomas, meningiomas and diverse benign tumors of the brain and other parts of the CNS., Results: During a median 11.3 years of follow-up, 328 women were diagnosed with CNS tumors. No marked associations were observed between use of the fertility drugs clomiphene citrate, gonadotropins, gonadotropin-releasing hormone receptor modulators and progesterone and CNS tumors. However, use of human chorionic gonadotropin was associated with a decreased rate of meningiomas (HR 0.49 95% CI 0.28-0.87). No clear associations with CNS tumors were observed according to time since first use or cumulative dose for any of the fertility drugs., Conclusion: No associations between use of most types of fertility drugs and CNS tumors were observed. However, our findings only apply to premenopausal women and additional studies with longer follow-up time are necessary., (© 2022. The Author(s), under exclusive licence to Springer Nature Switzerland AG.)

Published
2022
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197. Gene expression analysis during progression of malignant meningioma compared to benign meningioma.

Author

Maier AD, Meddis A, Mirian C, Haslund-Vinding J, Bartek J, Krog SM, Nguyen TUP, Areškevičiūtė A, Melchior LC, Heegaard S, Kristensen BW, Munch TN, Fugleholm K, Ziebell M, Raleigh DR, Poulsen FR, Gerds TA, Litman T, Scheie D, and Mathiesen T

Subjects
Humans, Gene Expression Profiling, Neoplasm Recurrence, Local pathology, Meningioma pathology, Meningeal Neoplasms pathology
Abstract

Objective: Meningioma is the most common primary intracranial neoplasm. Only 1%-3% of meningiomas are malignant according to the 2016 WHO criteria (WHO grade III). High-grade meningiomas present specific gene expression signatures indicating aggressive growth or recurrence. However, changes in gene expression and in neuroinflammatory gene expression signatures in WHO grade III meningiomas and during progression from WHO grade I or II to grade III are unknown., Methods: The authors used a NanoString targeted gene expression panel with focus on 787 genes relevant in meningioma pathology and neuroinflammatory pathways to investigate patients with grade III meningiomas treated at Rigshospitalet from 2000 to 2020 (n = 51). A temporal dimension was added to the investigation by including samples from patients' earlier grade I and II meningiomas and grade III recurrences (n = 139 meningiomas). The authors investigated changes in neuroinflammatory gene expression signatures in 1) grade I meningiomas that later transformed into grade III meningiomas, and 2) grade III meningiomas compared with nonrecurrent grade I meningiomas., Results: The authors' data indicate that FOXM1, TOP2A, BIRC5, and MYBL2 were enriched and the HOTAIR regulatory pathway was enriched in grade III meningiomas compared with nonrecurrent grade I meningiomas. They discovered a separation of malignant and benign meningiomas based only on genes involved in microglia regulation with enrichment of P2RY12 in grade I compared with grade III meningiomas. Interestingly, FOXM1 was upregulated in premalignant grade I meningioma years before the grade III transformation., Conclusions: The authors found gene expression changes in low-grade meningiomas that predated histological transformation to grade III meningiomas. Neuroinflammation genes distinguished grade III from grade I meningiomas.

Published
2022
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198. ISHLT consensus statement: Perioperative management of patients with pulmonary hypertension and right heart failure undergoing surgery.

Author

McGlothlin DP, Granton J, Klepetko W, Beghetti M, Rosenzweig EB, Corris PA, Horn E, Kanwar MK, McRae K, Roman A, Tedford R, Badagliacca R, Bartolome S, Benza R, Caccamo M, Cogswell R, Dewachter C, Donahoe L, Fadel E, Farber HW, Feinstein J, Franco V, Frantz R, Gatzoulis M, Hwa Anne Goh C, Guazzi M, Hansmann G, Hastings S, Heerdt PM, Hemnes A, Herpain A, Hsu CH, Kerr K, Kolaitis NA, Kukreja J, Madani M, McCluskey S, McCulloch M, Moser B, Navaratnam M, Rådegran G, Reimer C, Savale L, Shlobin OA, Svetlichnaya J, Swetz K, Tashjian J, Thenappan T, Vizza CD, West S, Zuckerman W, Zuckermann A, and De Marco T

Subjects
Consensus, Humans, Risk Assessment, Risk Factors, Heart Failure complications, Heart Failure surgery, Hypertension, Pulmonary epidemiology, Hypertension, Pulmonary surgery
Abstract

Pulmonary hypertension (PH) is a risk factor for morbidity and mortality in patients undergoing surgery and anesthesia. This document represents the first international consensus statement for the perioperative management of patients with pulmonary hypertension and right heart failure. It includes recommendations for managing patients with PH being considered for surgery, including preoperative risk assessment, planning, intra- and postoperative monitoring and management strategies that can improve outcomes in this vulnerable population. This is a comprehensive document that includes common perioperative patient populations and surgical procedures with unique considerations., (Copyright © 2022 International Society for Heart and Lung Transplantation. All rights reserved.)

Published
2022
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199. Pulmonary Vascular Research Institute GoDeep: A meta-registry merging deep phenotyping datafrom international PH reference centers.

Author

Majeed RW, Wilkins MR, Howard L, Hassoun PM, Anthi A, Cajigas HR, Cannon J, Chan SY, Damonte V, Elwing J, Förster K, Frantz R, Ghio S, Al Ghouleh I, Hilgendorff A, Jose A, Juaneda E, Kiely DG, Lawrie A, Orfanos SE, Pepe A, Pepke-Zaba J, Sirenko Y, Swett AJ, Torbas O, Zamanian RT, Marquardt K, Michel-Backofen A, Antoine T, Wilhelm J, Barwick S, Krieb P, Fuenderich M, Fischer P, Gall H, Ghofrani HA, Grimminger F, Tello K, Richter MJ, and Seeger W

Abstract

The Pulmonary Vascular Research Institute GoDeep meta-registry is a collaboration of pulmonary hypertension (PH) reference centers across the globe. Merging worldwide PH data in a central meta-registry to allow advanced analysis of the heterogeneity of PH and its groups/subgroups on a worldwide geographical, ethnical, and etiological landscape (ClinTrial. gov NCT05329714). Retrospective and prospective PH patient data (diagnosis based on catheterization; individuals with exclusion of PH are included as a comparator group) are mapped to a common clinical parameter set of more than 350 items, anonymized and electronically exported to a central server. Use and access is decided by the GoDeep steering board, where each center has one vote. As of April 2022, GoDeep comprised 15,742 individuals with 1.9 million data points from eight PH centers. Geographic distribution comprises 3990 enrollees (25%) from America and 11,752 (75%) from Europe. Eighty-nine perecent were diagnosed with PH and 11% were classified as not PH and provided a comparator group. The retrospective observation period is an average of 3.5 years (standard error of the mean 0.04), with 1159 PH patients followed for over 10 years. Pulmonary arterial hypertension represents the largest PH group (42.6%), followed by Group 2 (21.7%), Group 3 (17.3%), Group 4 (15.2%), and Group 5 (3.3%). The age distribution spans several decades, with patients 60 years or older comprising 60%. The majority of patients met an intermediate risk profile upon diagnosis. Data entry from a further six centers is ongoing, and negotiations with >10 centers worldwide have commenced. Using electronic interface-based automated retrospective and prospective data transfer, GoDeep aims to provide in-depth epidemiological and etiological understanding of PH and its various groups/subgroups on a global scale, offering insights for improved management., Competing Interests: AL has received support and fees from Janssen, Bayer, Novartis, GSK, Alexion, and IQVIA Ltd. DK has received personal fees for consultancy work giving education talks and participation in steering committees from Acceleron, Ferrer, GSK, and Janssen. His department has received grants for research from GSK and Janssen. EJ is GSL Investigator. HAG has received fees from Actelion, AstraZeneca, Bayer, GSK, Janssen‐Cilag, Lilly, Novartis, OMT, Pfizer, and United Therapeutics. HG has received fees from Actelion, AstraZeneca, Bayer, GSK, Janssen‐Cilag, Lilly, Novartis, OMT, Pfizer, and United Therapeutics. IAG has held research grants from the United Therapeutics and Gilead Sciences Research Scholars Programs. JC has served as a consultant for Acceleron Pharma, Actelion, GSK, and Merck and has received speaker fees from Actelion and GSK. JME has served as a consultant for United Therapeutics, Altavant, Aerovate, Bayer, Gossamer Bio, and Liquida. She has participated in clinical research funded by Janssen, United Therapeutics, Liquidia, Phase Bio, Gossamer Bio, Bayer, Acceleron, Altavant, and Aerovate. KT has received speaker fees from Janssen. MJR has received support from Janssen Pharmaceutica and Bayer Pharma AG, as well as speaker fees from Janssen Pharmaceutica and OMT. Stephen Y. Chan has served as a consultant for Acceleron Pharma and United Therapeutics; SYC (Stephen Y. Chan) has held research grants from Actelion, Bayer, and Pfizer. SYC has filed patent applications regarding metabolic targeting in pulmonary hypertension. SYC is a director, officer, and shareholder of Synhale Therapeutics. WS has received consultancy fees from Abivax, Lung Biotechnology, Liquidia, Medspray, Pieris, United Therapeutics, and Vectura. The remaining authors declare no conflict of interest., (© 2022 The Authors. Pulmonary Circulation published by John Wiley & Sons Ltd on behalf of Pulmonary Vascular Research Institute.)

Published
2022
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