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162


Distinctive Hypertrophic Cardiomyopathy Anatomy and Obstructive Physiology in Patients Admitted With Takotsubo Syndrome

Sherrid, Mark V; Riedy, Katherine; Rosenzweig, Barry; Massera, Daniele; Saric, Muhamed; Swistel, Daniel G; Ahluwalia, Monica; Arabadjian, Milla; DeFonte, Maria; Stepanovic, Alexandra; Serrato, Stephanie; Xia, Yuhe; Zhong, Hua; Maron, Martin S; Maron, Barry J; Reynolds, Harmony R
Clinical spectrum of hypertrophic cardiomyopathy (HC) has been expanded to include patients with mild or no thickening of the left ventricle (LV), who nevertheless have outflow tract obstruction at rest or after exercise, due to systolic anterior motion (SAM) and ventricular septal contact, with mitral valve elongation and papillary muscles anomalies. Apical ballooning mimicking a takotsubo syndrome (TS) wall motion pattern can occur in HC with mild septal thickening when latent obstruction becomes unrelenting. To define the prevalence of anatomic abnormalities characteristic of HC in patients diagnosed with TS, we analyzed echocardiograms of 44 unselected TS patients, age 67±12 years, 95% women including studies performed before the event (n = 11, median 515 days) and after recovery of left ventricular function (n = 33, median 92 days, interquartile range = 29 to 327) and compared the findings to 60 age and sexed matched controls. Analysis of echocardiograms was blinded to event timing, and patient vs. control status. During the ballooning event, 13 patients (30%) had SAM including 9 with LV outflow obstruction, peak gradients 71±40 mmHg, as well as: ventricular septal thickening (16 ± 4 mm), elongated anterior leaflets (30 ± 3mm), and increased mitral coaptation to posterior wall distance (17 ± 5 mm), consistent with diagnosis of the HC phenotype. Compared to 31 TS patients without SAM, study patients with SAM had longer anterior leaflets (30 ± 3 vs 26 ± 4 mm, p = 0.006), thicker septum (16 ± 4 vs 12 ± 3 mm), increased coaptation to posterior wall distance (17 ± 5 vs 14 ± 4 mm, p < 0.04) and reduced distance from coaptation to septum (19 ± 5 vs 27 ± 5, p < 0.001). In the 13 patients with SAM, morphologic characteristics of HC persisted after normalization of LV function. In conclusion, a subset of patients experiencing TS events demonstrates a constellation of morphologic abnormalities characteristic of HC that persist after recovery of LV wall motion. These findings suggest that dynamic outflow obstruction may cause apical ballooning in susceptible patients.
PMID: 32278461
ISSN: 1879-1913
CID: 4383042

Three-dimensional chromatin landscapes in T cell acute lymphoblastic leukemia

Kloetgen, Andreas; Thandapani, Palaniraja; Ntziachristos, Panagiotis; Ghebrechristos, Yohana; Nomikou, Sofia; Lazaris, Charalampos; Chen, Xufeng; Hu, Hai; Bakogianni, Sofia; Wang, Jingjing; Fu, Yi; Boccalatte, Francesco; Zhong, Hua; Paietta, Elisabeth; Trimarchi, Thomas; Zhu, Yixing; Van Vlierberghe, Pieter; Inghirami, Giorgio G; Lionnet, Timothee; Aifantis, Iannis; Tsirigos, Aristotelis
Differences in three-dimensional (3D) chromatin architecture can influence the integrity of topologically associating domains (TADs) and rewire specific enhancer-promoter interactions, impacting gene expression and leading to human disease. Here we investigate the 3D chromatin architecture in T cell acute lymphoblastic leukemia (T-ALL) by using primary human leukemia specimens and examine the dynamic responses of this architecture to pharmacological agents. Systematic integration of matched in situ Hi-C, RNA-seq and CTCF ChIP-seq datasets revealed widespread differences in intra-TAD chromatin interactions and TAD boundary insulation in T-ALL. Our studies identify and focus on a TAD 'fusion' event associated with absence of CTCF-mediated insulation, enabling direct interactions between the MYC promoter and a distal super-enhancer. Moreover, our data also demonstrate that small-molecule inhibitors targeting either oncogenic signal transduction or epigenetic regulation can alter specific 3D interactions found in leukemia. Overall, our study highlights the impact, complexity and dynamic nature of 3D chromatin architecture in human acute leukemia.
PMID: 32203470
ISSN: 1546-1718
CID: 4357602

Alvimopan for the Prevention of Postoperative Ileus in Inflammatory Bowel Disease Patients

Jang, Janice; Kwok, Benjamin; Zhong, Hua; Xia, Yuhe; Grucela, Alexis; Bernstein, Mitchell; Remzi, Feza; Hudesman, David; Chen, Jingjing; Axelrad, Jordan; Chang, Shannon
BACKGROUND:Postoperative ileus (POI) is a temporary delay of coordinated intestinal peristalsis. Alvimopan, an oral peripherally acting mu-opioid receptor antagonist approved for accelerating gastrointestinal recovery, has never been studied specifically in patients with inflammatory bowel disease (IBD). AIM/OBJECTIVE:To investigate the efficacy of alvimopan in preventing POI among IBD patients. METHODS:A retrospective chart review was conducted on 246 IBD patients undergoing bowel surgery between 2012 and 2017. Data collected included demographics, IBD subtype, length of stay (LOS), postoperative gastrointestinal symptoms, and administration of alvimopan. The primary outcome was POI; secondary gastrointestinal recovery outcomes were: time to first flatus, time to first bowel movement, time to tolerating a liquid diet, time to tolerating solid food, and LOS. RESULTS:When compared with the control group, patients in the alvimopan group had shorter times to tolerating liquids and solids, first flatus, and first bowel movements (p < 0.01). LOS was shorter in the alvimopan group when compared with controls (p < 0.01). The overall incidence of POI was higher in controls than in the alvimopan group (p = 0.07). For laparoscopic surgeries, the incidence of POI was also higher in controls than in the alvimopan group (p < 0.01). On multivariable analysis, alvimopan significantly decreased time to all gastrointestinal recovery endpoints when compared to controls (p < 0.01). CONCLUSIONS:Alvimopan is effective in accelerating time to gastrointestinal recovery and reducing POI in IBD patients. While the benefits of alvimopan have been demonstrated previously, this is the first study of the efficacy of alvimopan in IBD patients.
PMID: 31522323
ISSN: 1573-2568
CID: 4097752

Effects of Acute Colchicine Administration Prior to Percutaneous Coronary Intervention: COLCHICINE-PCI Randomized Trial

Shah, Binita; Pillinger, Michael; Zhong, Hua; Cronstein, Bruce; Xia, Yuhe; Lorin, Jeffrey D; Smilowitz, Nathaniel R; Feit, Frederick; Ratnapala, Nicole; Keller, Norma M; Katz, Stuart D
BACKGROUND:Vascular injury and inflammation during percutaneous coronary intervention (PCI) are associated with increased risk of post-PCI adverse outcomes. Colchicine decreases neutrophil recruitment to sites of vascular injury. The anti-inflammatory effects of acute colchicine administration before PCI on subsequent myocardial injury are unknown. METHODS:In a prospective, single-site trial, subjects referred for possible PCI (n=714) were randomized to acute preprocedural oral administration of colchicine 1.8 mg or placebo. RESULTS:=0.001). CONCLUSIONS:Acute preprocedural administration of colchicine attenuated the increase in interleukin-6 and high-sensitivity C-reactive protein concentrations after PCI when compared with placebo but did not lower the risk of PCI-related myocardial injury. Registration: URL: https://www.clinicaltrials.gov; Unique Identifiers: NCT02594111, NCT01709981.
PMID: 32295417
ISSN: 1941-7632
CID: 4383552

A NOVEL SUBSET OF HYPERTROPHIC CARDIOMYOPATHY PATIENTS CHARACTERIZED BY ASSOCIATION WITH TAKOTSUBO-LIKE LV BALLOONING AND HOSPITAL ADMISSION [Meeting Abstract]

Riedy, K N; Reynolds, H; Rosenzweig, B P; Massera, D; Saric, M; Swistel, D; Ahluwalia, M; Arabadjian, M; Defonte, M; Stepanovic, A; Serrato, S; Xia, Y; Zhong, H; Sherrid, M
Background Recently the clinical spectrum of hypertrophic cardiomyopathy (HCM) has been expanded to include patients with mild or no thickening of the left ventricle (LV) yet who have outflow tract obstruction at rest or after exercise, principally due to characteristic HCM anterior mitral leaflet (AML) elongation and papillary muscle anomalies. Apical ballooning mimicking a takotsubo syndrome (TTS) wall motion pattern can occur in mild-septal-thickening HCM when latent obstruction becomes unrelenting. The objective of this study is to define the prevalence of anatomic abnormalities characteristic of HCM in an unselected population of patients diagnosed clinically with TTS. Methods We analyzed echocardiograms of 44 admitted TTS patients including studies performed during admission, before the event (n=11, median 515 days before) and after recovery of left ventricular function (n=33, median 92 days, IQR=29-327) and compared them to 60 controls, age-matched normal women. Analysis of 148 echocardiograms was blinded to timing, and patient vs. control status. Results Age was 67+/-12 years, 42 female (95%). During the ballooning event, 13 (30%) had SAM and 9 patients (20%) had LV outflow tract obstruction (LVOTO), gradients 71+/-40 mmHg. Compared to TTS patients without SAM, those with SAM had longer AML (30 vs. 26mm), and thicker septum (16 vs. 12 mm) and less distance from septum to coaptation (19 vs. 27mm), all p <=0.006. Eleven of the SAM patients had >=2 anatomic abnormalities predisposing to obstruction (defined as > 2 SD above normal), and/or an anomalous papillary muscle/chordae. In the 44 TTS patients each parameter differed from controls before, during and after the TTS event. Eight (18%) had abnormal right ventricular wall motion, none of whom were obstructed. Conclusion Thirty percent of unselected TTS patients have SAM and 20% have significant LVOT gradients. This subset had AML abnormalities and septal thickening typical of obstructive HCM and known to predispose to LVOT obstruction. They are phenotypically identical to patients with documented HCM with mild septal thickening and LVOT obstruction, who have experienced episodes of ballooning.
EMBASE:2005041582
ISSN: 0735-1097
CID: 4367622

ERAP1-MEDIATED IMMUNOGENICITY AND IMMUNEPHENOTYPES IN HLA-B51+BEHCET'S DISEASE POINT TO PATHOGENIC CD8 T CELL EFFECTOR RESPONSES [Meeting Abstract]

Al-Obeidi, A. F.; Cavers, A.; Ozguler, Y.; Manches, O.; Zhong, H.; Yurttas, B.; Ueberheide, B.; Hatemi, G.; Kugler, M.; Nowatzky, J.
ISI:000555905000034
ISSN: 0003-4967
CID: 4562812

Coronary OCT and Cardiac MRI to Determine Underlying Causes of Minoca in Women [Meeting Abstract]

Reynolds, Harmony; Maehara, Akiko; Kwong, Raymond; Sedlak, Tara; Saw, Jacqueline; Smilowitz, Nathaniel; Mahmud, Ehtisham; Wei, Janet; Marzo, Kevin; Matsumura, Mitsuaki; Seno, Ayako; Hausvater, Anais; Giesler, Caitlin; Jhalani, Nisha; Toma, Catalin; Har, Bryan; Thomas, Dwithiya; Mehta, Laxmi S.; Trost, Jeffrey; Mehta, Puja; Ahmed, Bina; Bainey, Kevin R.; Xia, Yuhe; Shah, Binita; Attubato, Michael; Bangalore, Sripal; Razzouk, Louai; Ali, Ziad; Merz, Noel Bairey; Park, Ki; Hada, Ellen; Zhong, Hua; Hochman, Judith S.
ISI:000639226400050
ISSN: 0009-7322
CID: 5285732

ERAP1-mediated immunogenicity and immune-phenotypes in HLA-B51(+) Behcet's and Behcet's uveitis point to pathogenic CD8 T cell effector responses [Meeting Abstract]

Nowatzky, Johannes; Cavers, Ann; Ozguler, Yesim; Al-Obeidi, Arshed Fahad; Yurttas, Berna; Zhong, Hua; Xia, Yuhe; Ueberheide, Beatrix; Hatemi, Gulen; Kugler, Matthias; Manches, Olivier
ISI:000554528303086
ISSN: 0146-0404
CID: 5340352

A phase II, randomized, controlled trial of nivolumab in combination with BMS-986253 or cabiralizumab in advanced hepatocellular carcinoma (HCC) patients [Meeting Abstract]

Welling, T; Beri, N; Siolas, D; Cohen, D J; Becker, D J; Zhong, H; Wu, J J; Oberstein, P E; Karasic, T B
Background: Tyrosine kinase inhibitors can prolong survival in advanced HCC patients, but response rates have been minimal. Recently, immune checkpoint inhibition with nivolumab (nivo) demonstrated objective response rates (ORR) of 15% (escalation phase) and 20% (expansion phase) in the Checkmate 040 study. Pre-clinical and translational studies have demonstrated that IL-8 and tumor associated macrophages (TAMs) contribute to HCC progression and recurrence following treatment. Therefore, rationale exists to evaluate combinatorial approaches to target TAM function combined with checkpoint inhibitory therapy. This phase II, randomized study will evaluate the safety and efficacy of combined anti-CSF1R (Cabiralizumab) or anti-IL-8 (BMS-986253) in combination with Nivo in advanced HCC. Method(s): Advanced HCC patients without prior systemic treatment and disease measurable by RECISTv1.1 with Childs A liver function are eligible. Patients will be enrolled (n=25 per arm) to Nivo 240 mg IV Q2 weeks monotherapy, Nivo 240 mg IV + BMS-986253 1200 mg IV Q2 weeks, or Nivo 240 mg IV + Cabiralizumab 4 mg/kg IV Q2 weeks. Primary endpoints include safety and ORR determined by RECISTv1.1. Secondary endpoints include time to response, duration of response, progression free survival, and overall survival. Exploratory endpoints include analysis of tumor microenvironment immune and tumor cell profiling of pre- and on-treatment tumor tissue
EMBASE:630962090
ISSN: 1527-7755
CID: 4326202

ERAP1-mediated Immunogenicity and Immune-phenotypes in HLA-B51+Behcet's Disease Point to Pathogenic CD8 T Cell Effector Responses [Meeting Abstract]

Cavers, Ann; Ozguler, Yesim; Manches, Olivier; Al-Obeidi, Arshed; Zhong, Hua; Ueberheide, Beatrix; Hatemi, Gulen; Kugler, Matthias; Nowatzky, Johannes
ISI:000587568501022
ISSN: 2326-5191
CID: 5340362