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48


Growth of liver allografts over time in pediatric transplant recipients

Chaudhry, S G; Bentley-Hibbert, S; Stern, J; Lobritto, S; Martinez, M; Vittorio, J; Halazun, K J; Lee, H T; Emond, J; Kato, T; Samstein, B; Griesemer, A
The liver's capacity to grow in response to metabolic need is well known. However, long-term growth of liver allografts in pediatric recipients has not been characterized. A retrospective review of pediatric recipients at a single institution identified patients who had cross-sectional imaging at 1, 5, and 10 years post-transplant. Using volumetric calculations, liver allograft size was calculated and percent SLV were compared across the different time points; 18 patients ranging from 0.3 to 17.7 years old were identified that had imaging at 2 or more time points. Measured liver volumes increased by 59% after 5 years and 170% after 10 years. The measured liver volumes compared to calculated %SLV for these patients were 123 ± 37%, 97 ± 19%, and 118 ± 27% at 1, 5, and 10 years after transplant, respectively. Our data suggest that liver allografts in pediatric recipients increase along with overall growth, and reach SLVs for height and weight by 5 years post-transplantation. Additionally, as pediatric recipients grow, the livers appear to maintain appropriate SLV.
PMCID:5820167
PMID: 29334158
ISSN: 1399-3046
CID: 5161192

Enteric serotonin and oxytocin: endogenous regulation of severity in a murine model of necrotizing enterocolitis

Gross Margolis, Kara; Vittorio, Jennifer; Talavera, Maria; Gluck, Karen; Li, Zhishan; Iuga, Alina; Stevanovic, Korey; Saurman, Virginia; Israelyan, Narek; Welch, Martha G; Gershon, Michael D
Necrotizing enterocolitis (NEC), a gastrointestinal inflammatory disease of unknown etiology that may also affect the liver, causes a great deal of morbidity and mortality in premature infants. We tested the hypothesis that signaling molecules, which are endogenous to the bowel, regulate the severity of intestinal and hepatic damage in an established murine NEC model. Specifically, we postulated that mucosal serotonin (5-HT), which is proinflammatory, would exacerbate experimental NEC and that oxytocin (OT), which is present in enteric neurons and is anti-inflammatory, would oppose it. Genetic deletion of the 5-HT transporter (SERT), which increases and prolongs effects of 5-HT, was found to increase the severity of systemic manifestations, intestinal inflammation, and associated hepatotoxicity of experimental NEC. In contrast, genetic deletion of tryptophan hydroxylase 1 (TPH1), which is responsible for 5-HT biosynthesis in enterochromaffin (EC) cells of the intestinal mucosa, and TPH inhibition with LP-920540 both decrease the severity of experimental NEC in the small intestine and liver. These observations suggest that 5-HT from EC cells helps to drive the inflammatory damage to the gut and liver that occurs in the murine NEC model. Administration of OT decreased, while the OT receptor antagonist atosiban exacerbated, the intestinal inflammation of experimental NEC. Data from the current investigation are consistent with the tested hypotheses-that the enteric signaling molecules, 5-HT (positively) and OT (negatively) regulate severity of inflammation in a mouse model of NEC. Moreover, we suggest that mucosally restricted inhibition of 5-HT biosynthesis and/or administration of OT may be useful in the treatment of NEC.NEW & NOTEWORTHY Serotonin (5-HT) and oxytocin reciprocally regulate the severity of intestinal inflammation and hepatotoxicity in a murine model of necrotizing enterocolitis (NEC). Selective depletion of mucosal 5-HT through genetic deletion or inhibition of tryptophan hydroxylase-1 ameliorates, while deletion of the 5-HT uptake transporter, which increases 5-HT availability, exacerbates the severity of NEC. In contrast, oxytocin reduces, while the oxytocin receptor antagonist atosiban enhances, NEC severity. Peripheral tryptophan hydroxylase inhibition may be useful in treatment of NEC.
PMID: 28774871
ISSN: 1522-1547
CID: 5230562

Anakinra-Induced Acute Liver Failure in an Adolescent Patient with Still's Disease [Case Report]

Taylor, Sarah A; Vittorio, Jennifer M; Martinez, Mercedes; Fester, Keith A; Lagana, Stephen M; Lobritto, Steven J; Ovchinsky, Nadia
The interleukin-1 (IL-1) family consists of 11 cytokines that play key regulatory roles in many immune and inflammatory processes. Anakinra (Kineret, Amgen, Inc.) is an IL-1 receptor antagonist (IL-1ra). Increased levels of IL-1 are found in several disease states suggesting that anakinra may be beneficial in disorders associated with elevated IL-1 levels. Anakinra has been effectively used in the treatment of systemic juvenile idiopathic arthritis and adult-onset Still's disease (AOSD). Despite its therapeutic benefits, anakinra also has potential side effects, including hepatotoxicity. We present a case of AOSD in an adolescent male that was treated with anakinra. During treatment, the patient developed acute liver failure that resolved upon withdrawal of anakinra. Although anakinra-induced liver injury has been reported in adults, including one case of subacute liver failure, we believe our case is the first to show severe acute liver failure in an adolescent treated with anakinra. This case provides significant insight into a potentially serious complication associated with anakinra. It is important to further delineate these complications as the treatment indications for this drug expand.
PMID: 26749403
ISSN: 1875-9114
CID: 5397292

Immunologic Advantage of Maternal Grafts in Pediatric Living Donor Liver Transplantation (LDLT) [Meeting Abstract]

Przybyszewski, Eric; Verna, Elizabeth C.; Lobritto, Steven J.; Martinez, Mercedes; Vittorio, Jennifer; Fox, Alyson N.; Samstein, Benjamin; Kato, Tomoaki; Griesemer, Adam D.; Emond, Jean C.
ISI:000385493800216
ISSN: 0270-9139
CID: 5397402

Outcomes of Liver Transplantation in Children Younger Than One Year of Age [Meeting Abstract]

Kinberg, Sivan; Vittorio, Jennifer; Griesemer, Adam; Kato, Tomoaki; Lobritto, Steven J.; Martinez, Mercedes
ISI:000360120300600
ISSN: 0016-5085
CID: 5397392

Low Rate of Recurrent Primary Sclerosing Cholangitis in Pediatric Orthotopic Liver Transplant Recipients [Meeting Abstract]

Taylor, Sarah; Lobritto, Steven J.; Martinez, Mercedes; Vittorio, Jennifer; Griesemer, Adam; Kato, Tomoaki; Emond, Jean C.; Ovchinsky, Nadia
ISI:000344483804165
ISSN: 0270-9139
CID: 5397382

Serotonin promotes periportal inflammation and fatty infiltration of the liver in a murine model of necrotizing enterocolitis [Meeting Abstract]

Vittorio, Jennifer; Stevanovic, Korey; Li, Zhishan; Gershon, Michael D.; Margolis, Kara
ISI:000310955601015
ISSN: 0270-9139
CID: 5397372

Serotonin Plays a Proinflammatory Role in Murine Necrotizing Enterocolitis [Meeting Abstract]

Margolis, Kara G.; Talavera, Maria; Stevanovic, Korey D.; Yang, Qi M.; Li, Zhishan; Kim, Soyoun Rosa; Diacou, Alexander; Vittorio, Jennifer; Bednarz, Mark S.; Gershon, Michael D.
ISI:000306994300475
ISSN: 0016-5085
CID: 5397362