Alcohol intoxication complicates injury and infection by impairing cardiovascular function, fluid homeostasis, and host defense. The lymphatics of the gut are a multifunctional transport system that normally serves as a delivery and surveillance system for potentially harmfull antigens, optimizing mucosal innate and adaptative immunity. Alcohol increases mesenteric lymph flow, which could potentially be harmful if gut barrier function is compromised, such as after traumatic injury. In such cases increased lymph flow could facilitate delivery of an overwhelming number of pathogens to the lymph node barrier, allowing entry to the systemic circulation, and infection of the heart, lungs and other organs. We recently showed that alcohol modulates the intrinsic contractile cycle of mesenteric lymphatics that provides the driving force for lymph flow.
We aim to discover the molecular mechanisms by which alcohol enhances intrinsic lymphatic pumping. Because of the known importance of Ca[2+] in smooth muscle contraction, we developed a novel method to measure cytosolic [Ca[2+]] in isolated rat collecting lymphatics. Our preliminary data indicate that alcohol modulates phasic contractions of lymphatic vessels by decreasing the frequency yet increasing the magnitude of cyclic mobilizations of Ca[2+] from internal stores. Alcohol also inhibits the lymphatic myogenic constriction in response to increases in luminal pressure. However, alcohol does not inhibit the associated gradual increase in cytosolic [Ca[2+]] during the diastolic phase of the contractile cycle, which suggests that the inhibition of myogenic constriction may instead be due to impaired sensitivity to Ca[2+]. We hypothesize that alcohol decreases the frequency and increases the magnitude of Ca[2+] mobilization in lymphatic smooth muscle to cause less frequent but larger contractions, and in addition decreases mesenteric lymphatic tone by inhibiting Ca[2+]-sensitizing mechanisms. We will test this hypothesis with two Specific Aims: 1) to test the prediction that acute alcohol intoxication induced-changes in the lymphatic phasic contraction pattern are caused by an altered cyclic mobilization of Ca[2+], and 2) to demonstrate that alcohol intoxication inhibits Ca[2+] sensitization in lymphatic smooth muscle, causing a decrease in tone and loss of myogenic responsiveness. We will utilize an established rat model of acute alcohol intoxication in combination with our novel method to simultaneously track changes in cytosolic [Ca[2+]] and intrinsic pump function in isolated mesenteric lymphatics. In addition, pharmacological interventions will be combined with biochemical analyses of key signaling molecules to determine the underlying Ca[2+]- dependent and Ca[2+]-sensitizing mechanisms impacted by alcohol intoxication. The successful completion of these studies will reveal the lymphatic contractile mechanisms impacted by alcohol intoxication, this will advance our knowledge on how alcohol intoxication disrupts immunity in the digestive tract. This information will also enable development of useful therapeutic strategies to prevent infections that hamper cardio- pulmonary function in alcohol-intoxicated trauma victims.

Public Health Relevance

Alcohol intoxication complicates injury and infection by impairing cardiovascular function, fluid balance, and immunity. In the traumatically injured, alcohol intoxicated host, alcohol-induced enhancement of mesenteric lymph flow could potentially increase the transport of an overwhelming number of pathogens through the lymph node barrier and into the systemic circulation, allowing infection of the heart, lungs and other organs. We aim to discover the molecular mechanisms in the gut lymphatic vessels that could potentially serve as therapeutic targets in the development of succesful clinical strategies to limt the development of infections.

Agency
National Institute of Health (NIH)
Institute
National Institute on Alcohol Abuse and Alcoholism (NIAAA)
Type
Postdoctoral Individual National Research Service Award (F32)
Project #
1F32AA021049-01A1
Application #
8314893
Study Section
Health Services Research Review Subcommittee (AA)
Program Officer
Jung, Kathy
Project Start
2012-03-15
Project End
2015-03-14
Budget Start
2012-03-15
Budget End
2013-03-14
Support Year
1
Fiscal Year
2012
Total Cost
$52,190
Indirect Cost
Name
Louisiana State Univ Hsc New Orleans
Department
Physiology
Type
Schools of Medicine
DUNS #
782627814
City
New Orleans
State
LA
Country
United States
Zip Code
70112
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Souza-Smith, Flavia M; Kerut, Edmund K; Breslin, Jerome W et al. (2015) Mechanisms of Acute Alcohol Intoxication-Induced Modulation of Cyclic Mobilization of [Ca²?] in Rat Mesenteric Lymphatic Vessels. Lymphat Res Biol 13:93-9
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Kurtz, Kristine H; Souza-Smith, Flavia M; Moor, Andrea N et al. (2014) Rho kinase enhances contractions of rat mesenteric collecting lymphatics. PLoS One 9:e94082
Souza-Smith, Flavia M; Molina, Patricia E; Breslin, Jerome W (2012) Reduced RhoA activity mediates acute alcohol intoxication-induced inhibition of lymphatic myogenic constriction despite increased cytosolic [Ca(2+) ]. Microcirculation :