Mitochondrial Targeting Therapy Role it Liver Transplant Preservation Lines: Mechanism and Therapeutic Strategies

被引:8
作者
Tara, Anjli [1 ,2 ]
Dominic, Jerry Lorren [1 ,3 ,4 ,5 ]
Patel, Jaimin N. [6 ]
Garg, Ishan [7 ]
Yeon, Jimin [7 ]
Memon, Marrium S. [8 ]
Rao, Sanjay Rao Gergal Gopalkrishna [9 ]
Bugazia, Seif [10 ]
Dhandapani, Tamil Poonkuil Mozhi [11 ,12 ]
Kannan, Amudhan [13 ,14 ]
Kantamaneni, Ketan [15 ,16 ]
Win, Myat [1 ,17 ]
Went, Terry R. [15 ]
Yanamala, Vijaya Lakshmi [15 ]
Mostafa, Jihan A. [18 ]
机构
[1] Calif Inst Behav Neurosci & Psychol CIBNP, Gen Surg, Fairfield, CA 94534 USA
[2] Liaquat Univ Med & Hlth Sci LUMHS, Gen Surg, Jamshoro, Pakistan
[3] Vinayaka Missions Kirupananda Variyar Med Coll, Gen Surg, Salem, India
[4] Stony Brook Southampton Hosp, Gen Surg, New York, NY USA
[5] Cornerstone Reg Hosp, Gen Surg & Orthopaed Surg, Edinburg, TX USA
[6] Calif Inst Behav Neurosci & Psychol CIBNP, Family Med, Fairfield, CA USA
[7] Calif Inst Behav Neurosci & Psychol CIBNP, Med, Fairfield, CA USA
[8] Calif Inst Behav Neurosci & Psychol CIBNP, Res, Fairfield, CA USA
[9] Calif Inst Behav Neurosci & Psychol CIBNP, Internal Med, Fairfield, CA USA
[10] Calif Inst Behav Neurosci & Psychol CIBNP, Fac Med, Fairfield, CA USA
[11] Calif Inst Behav Neurosci & Psychol CIBNP, Internal Med Family Med, Fairfield, CA USA
[12] Med City Plano, Internal Med, Plano, TX USA
[13] Jawaharlal Inst Postgrad Med Educ & Res JIPMER, Med, Pondicherry, India
[14] Calif Inst Behav Neurosci & Psychol CIBNP, Gen Surg Res, Fairfield, CA USA
[15] Calif Inst Behav Neurosci & Psychol CIBNP, Surg, Fairfield, CA USA
[16] Dr Pinnamaneni Siddhartha Inst Med Sci & Res Fdn, Surg, Gannavaram, India
[17] Nottingham Univ Hosp NHS Trust, Gen Surg, Nottingham, England
[18] Calif Inst Behav Neurosci & Psychol CIBNP, Psychiat & Behav Sci, Fairfield, CA USA
关键词
liver transplantation; mitochondrial targeting therapy; pathophysiology; ischemiaireperfusion injury; mechanism; preservation; therapeutics; graft survival; graft failure; ISCHEMIA-REPERFUSION INJURY; HEPATIC ISCHEMIA; MACHINE PERFUSION; PROTECTION; PATHWAY; RATS;
D O I
10.7759/cureus.16599
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
The normal function of mitochondria in the hepatic parenchyma can be disrupted by ischemia/reperfusion (l/R) damage during liver transplantation. The pathology of these insults involves various cellular and molecular steps of events that have been extensively researched over decades but are yet to provide complete answers. This review discusses the brief mechanism of the pathophysiology following ischemia/reperfusion injury (IRI) and various targeting strategies that could result in improved graft function. The traditional treatment for end-stage liver disease i.e., liver transplantation, has been complicated by I/R damage. The poor graft function or primary non-function found after liver transplantation may be due to mitochondria! dysfunction following IRI. As a result, determining the sequence of incidents that cause human hepatic mitochondria! dysfunction is crucial; it might contribute to further improvements in the outcome of liver transplantation. Early discovery of novel prognostic factors involved in IRI could serve as a primary endpoint for predicting the outcome of liver grafts as well as promoting the early implementation of novel IRI-prevention strategies. In this review, recent developments in the study of mitochondrial dysfunction and I/R damage are discussed, specifically those concerning liver transplantation. Furthermore, we also explore different pharmacological therapeutic methods that may be used and their connections to mitochondrion-related processes and goals. Although significant progress has been made in our understanding of IRI and mitochondrial dysfunction, further research is needed to elucidate the cellular and molecular pathways underlying these processes to help identify biomarkers that can aid donor organ evaluation.
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页数:9
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