Increased susceptibility to ischemia causes exacerbated response to microinjuries in the cirrhotic liver

Author:

Leaker Ben D.12ORCID,Sojoodi Mozhdeh34ORCID,Tanabe Kenneth K.34ORCID,Popov Yury V.56ORCID,Tam Joshua27ORCID,Anderson R. Rox27ORCID

Affiliation:

1. Health Sciences and Technology Harvard‐Massachusetts Institute of Technology Cambridge Massachusetts USA

2. Wellman Center for Photomedicine Massachusetts General Hospital Boston Massachusetts USA

3. Division of Gastrointestinal and Oncologic Surgery Massachusetts General Hospital Boston Massachusetts USA

4. Department of Surgery Harvard Medical School Boston Massachusetts USA

5. Division of Gastroenterology, Hepatology and Nutrition Beth Israel Deaconess Medical Center Boston Massachusetts USA

6. Department of Medicine Harvard Medical School Boston Massachusetts USA

7. Department of Dermatology Harvard Medical School Boston Massachusetts USA

Abstract

AbstractFractional laser ablation is a technique developed in dermatology to induce remodeling of skin scars by creating a dense pattern of microinjuries. Despite remarkable clinical results, this technique has yet to be tested for scars in other tissues. As a first step toward determining the suitability of this technique, we aimed to (1) characterize the response to microinjuries in the healthy and cirrhotic liver, and (2) determine the underlying cause for any differences in response. Healthy and cirrhotic rats were treated with a fractional laser then euthanized from 0 h up to 14 days after treatment. Differential expression was assessed using RNAseq with a difference‐in‐differences model. Spatial maps of tissue oxygenation were acquired with hyperspectral imaging and disruptions in blood supply were assessed with tomato lectin perfusion. Healthy rats showed little damage beyond the initial microinjury and healed completely by 7 days without scarring. In cirrhotic rats, hepatocytes surrounding microinjury sites died 4‐6 h after ablation, resulting in enlarged and heterogeneous zones of cell death. Hepatocytes near blood vessels were spared, particularly near the highly vascularized septa. Gene sets related to ischemia and angiogenesis were enriched at 4 h. Laser‐treated regions had reduced oxygen saturation and broadly disrupted perfusion of nodule microvasculature, which matched the zones of cell death. Our results demonstrate that the cirrhotic liver has an exacerbated response to microinjuries and increased susceptibility to ischemia from microvascular damage, likely related to the vascular derangements that occur during cirrhosis development. Modifications to the fractional laser tool, such as using a femtosecond laser or reducing the spot size, may be able to prevent large disruptions of perfusion and enable further development of a laser‐induced microinjury treatment for cirrhosis.

Publisher

Wiley

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