Aakash Nagarapu scite author profile

Aakash Nagarapu

4Publications

7Citation Statements Received

237Citation Statements Given

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160

227

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Saint Louis University

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Novel Therapeutic Approaches for Mitigating Complications in Short Bowel Syndrome

Bettag

Cunningham

et al. 2022

Nutrients

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Short bowel syndrome (SBS) is a particularly serious condition in which the small intestine does not absorb sufficient nutrients for biological needs, resulting in severe illness and potentially death if not treated. Given the important role of the gut in many signaling cascades throughout the body, SBS results in disruption of many pathways and imbalances in various hormones. Due to the inability to meet sufficient nutritional needs, an intravenous form of nutrition, total parental nutrition (TPN), is administered. However, TPN presents difficulties such as severe liver injury and altered signaling secondary to the continued lack of luminal contents. This manuscript aims to summarize relevant studies into the systemic effects of TPN on systems such as the gut–brain, gut-lung, and gut-liver axis, as well as present novel therapeutics currently under use or investigation as mitigation strategies for TPN induced injury.

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Carbamazepine mitigates parenteral nutrition–associated liver disease in a novel ambulatory piglet model

Song

Nagarapu

Nispen

et al. 2022

J Parenter Enteral Nutr

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Background Parenteral nutrition (PN) remains a critical therapeutic option in patients who cannot tolerate enteral feeding. However, although lifesaving, PN is associated with significant side effects, including liver injury, the etiology of which is multifactorial. Carbamazepine (CBZ), an antiepileptic medication, is known to modulate hepatic fibrosis and hepatocellular injury in a variety of liver diseases. We hypothesized that CBZ could prevent PN‐associated liver disease (PNALD), which we tested by using our novel ambulatory PN piglet model. Methods Piglets were fitted with jugular catheters and infusion pumps for PN and randomized to enteral nutrition (n = 7), PN (n = 6), or PN with parenteral CBZ (n = 6) for 2 weeks. Serum and liver tissue were analyzed via light microscopy, quantification of serum liver injury markers, Ki67 and cytokeratin‐7 indexing, and real‐time quantitative polymerase chain reaction. Results PN‐fed piglets in our model developed manifestations of PNALD—particularly, increased serum bilirubin, gamma‐glutamyltransferase, liver cholestasis, and Ki67 expression compared with that of EN‐fed animals (P < 0.03). CBZ therapy in PN‐fed animals led to a significant reduction in these markers of injury (P < 0.05). Investigation into the mechanism of these therapeutic effects revealed increased expression of sterol regulatory element‐binding protein 1 (SREBP‐1), peroxisome proliferator‐activated receptor alpha (PPAR‐α), and fatty acid binding protein (FABP) in PN‐fed animals receiving CBZ (P < 0.03). Further investigation revealed increased LC3 expression and decreased lysosomal‐associated membrane protein (LAMP1) expression with CBZ (P < 0.03). Conclusion CBZ administration mitigates PNALD severity, suggesting a novel therapeutic strategy targeting PN‐associated side effects, and may present a paradigm change to current treatment options.

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711: Autologous Internal Recirculation of Distal Intestinal Content Mitigates Liver and Gut Injury in a Novel Piglet Short Bowel Syndrome Model

Hutchinson¹,

Nispen²,

Samaddar³

et al. 2022

Gastroenterology

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Ep1212: A Histopathological Assessment of Total Parenteral Nutrition Driven Immune Dysfunction in a Novel Neonatal Pig Model

Chen¹,

Hutchinson²,

Besmer³

et al. 2022

Gastroenterology

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Aakash Nagarapu

Novel Therapeutic Approaches for Mitigating Complications in Short Bowel Syndrome

Carbamazepine mitigates parenteral nutrition–associated liver disease in a novel ambulatory piglet model

711: Autologous Internal Recirculation of Distal Intestinal Content Mitigates Liver and Gut Injury in a Novel Piglet Short Bowel Syndrome Model

Ep1212: A Histopathological Assessment of Total Parenteral Nutrition Driven Immune Dysfunction in a Novel Neonatal Pig Model

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