Lymphangiogenesis and Lymphatic Barrier Dysfunction in Renal Fibrosis

Liu, Jing; Chen, Yu

doi:10.3390/ijms23136970

Cited by 11 publications

(17 citation statements)

References 117 publications

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“…[86][87][88][89] Together with soluble factors, tissue stiffening produces pathological vasculature with altered lymph fluid flow characteristics and transmural transport properties that maintain or worsen the disease state. [8][9][10][11]76,77,80] Moreover, increased lymphatic vascularization can promote fibrosis via a positive feedback loop, [12,23,83,[90][91][92] and when rapid lymphangiogenesis occurs, vascular permeability (i.e., barrier function) can increase [21,23,93] and produce leaky, nonfunctional vessels. [29,87,94] Conversely, there are disease states with significant fibrosis (e.g., secondary lymphedema, myocardial edema) and insufficient lymphatic vasculature (i.e., inadequate growth, low number of vessels, low vessel function).…”

Section: Fibrosis Inflammation and Lymphaticsmentioning

confidence: 99%

“…[26][27][28] In chronic kidney disease with renal fibrosis, increased lymphangiogenesis helps drain excess fluid, but increased recruitment of dendritic cells to the lymph nodes combined with leaky vessels disrupts the immune response. [10,13] Since inflammation and tissue stiffening can trigger lymphangiogenesis and alter barrier function, [14,16,20,29,30] studies on lymphatic vasculature should consider each of these factors when developing therapeutic strategies. Currently, there are differences in treatment approaches based on the type of lymphatic dysregulation.…”

Section: Introductionmentioning

confidence: 99%

“…[ 26–28 ] In chronic kidney disease with renal fibrosis, increased lymphangiogenesis helps drain excess fluid, but increased recruitment of dendritic cells to the lymph nodes combined with leaky vessels disrupts the immune response. [ 10,13 ]…”

Section: Introductionmentioning

confidence: 99%

“…[7] Fibrosis-excess extracellular matrix (ECM) deposition and scarring of connective tissue-is a common occurrence across numerous pathological conditions that also involve significant amount of lymphatic dysregulation (e.g., chronic kidney disease, lymphedema, cardiac fibrosis, cancerous tumors). [8][9][10][11][12][13] Inflammation often works in tandem with fibrosis in many conditions to create a biophysical (e.g., ECM stiffening), biomechanical (e.g., increased interstitial pressure), and biochemical (e.g., pro-lymphangiogenic growth factors, inflammatory cytokines) environment that changes with time and perpetuates the disease state. [8,[14][15][16][17][18] These changes not only influence lymphatic endothelial cell (LEC) behavior (i.e., proliferation, migration) and cell-cell junction integrity, [2,19,20] but they also affect stromal cell populations (e.g., fibroblasts, immune cells) that interact with LECs through paracrine signaling.…”

mentioning

confidence: 99%

“…Adv. Biology 2023,7, 2200158 • Excess lymphatic growth in response to fibrosis can cause organ function disruption (e.g., kidney ultrafiltration) • Aberrant mural cell recruitment causes vascular remodeling of the lymphatic tissue • Lymphatic vasculature recruits immune cells, aggravating the inflammatory response and further progressing fibrosis[4,10,82,125] …”

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confidence: 99%

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Regulating Lymphatic Vasculature in Fibrosis: Understanding the Biology to Improve the Modeling

Ruliffson

Whittington

2023

Advanced Biology

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Fibrosis occurs in many chronic diseases with lymphatic vascular insufficiency (e.g., kidney disease, tumors, and lymphedema). New lymphatic capillary growth can be triggered by fibrosis‐related tissue stiffening and soluble factors, but questions remain for how related biomechanical, biophysical, and biochemical cues affect lymphatic vascular growth and function. The current preclinical standard for studying lymphatics is animal modeling, but in vitro and in vivo outcomes often do not align. In vitro models can also be limited in their ability to separate vascular growth and function as individual outcomes, and fibrosis is not traditionally included in model design. Tissue engineering provides an opportunity to address in vitro limitations and mimic microenvironmental features that impact lymphatic vasculature. This review discusses fibrosis‐related lymphatic vascular growth and function in disease and the current state of in vitro lymphatic vascular models while highlighting relevant knowledge gaps. Additional insights into the future of in vitro lymphatic vascular models demonstrate how prioritizing fibrosis alongside lymphatics will help capture the complexity and dynamics of lymphatics in disease. Overall, this review aims to emphasize that an advanced understanding of lymphatics within a fibrotic disease—enabled through more accurate preclinical modeling—will significantly impact therapeutic development toward restoring lymphatic vessel growth and function in patients.

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Section: Fibrosis Inflammation and Lymphaticsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Regulating Lymphatic Vasculature in Fibrosis: Understanding the Biology to Improve the Modeling

Ruliffson

Whittington

2023

Advanced Biology

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Kidney Lymphatics

Russell

Itkin

Windsor

et al. 2023

Comprehensive Physiology

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Eplerenone reduces lymphangiogenesis in the contralateral kidneys of UUO rats

Hao,

Qiang,

Fan

et al. 2024

Sci Rep

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Inflammation and fibrosis often occur in the kidney after acute injury, resulting in chronic kidney disease and consequent renal failure. Recent studies have indicated that lymphangiogenesis can drive renal inflammation and fibrosis in injured kidneys. However, whether and how this pathogenesis affects the contralateral kidney remain largely unknown. In our study, we uncovered a mechanism by which the contralateral kidney responded to injury. We found that the activation of mineralocorticoid receptors and the increase in vascular endothelial growth factor C in the contralateral kidney after unilateral ureteral obstruction could promote lymphangiogenesis. Furthermore, mineralocorticoid receptor activation in lymphatic endothelial cells resulted in the secretion of myofibroblast markers, thereby contributing to renal fibrosis. We observed that this process could be attenuated by administering the mineralocorticoid receptor blocker eplerenone, which, prevented the development of fibrotic injury in the contralateral kidneys of rats with unilateral ureteral obstruction. These findings offer valuable insights into the intricate mechanisms underlying kidney injury and may have implications for the development of therapeutic strategies to mitigate renal fibrosis in the context of kidney disease.

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Lymphangiogenesis and Lymphatic Barrier Dysfunction in Renal Fibrosis

Cited by 11 publications

References 117 publications

Regulating Lymphatic Vasculature in Fibrosis: Understanding the Biology to Improve the Modeling

Regulating Lymphatic Vasculature in Fibrosis: Understanding the Biology to Improve the Modeling

Kidney Lymphatics

Eplerenone reduces lymphangiogenesis in the contralateral kidneys of UUO rats

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