Rejection Sensitivity and Support Seeking Among the Stigmatized

LaDuke, Sheri L., Williams, Stacey L.

01 August 2014

No description available.

rejection

sensitivity

support

stigmatized

Psychology

Image Is Everything: Self-Presentation Following Social Exclusion

Tuscherer, Taylor R.

07 December 2012

No description available.

Social Psychology

reaffiliation

rejection

belongingness

Why was I Rejected? How the Attributed Reason for Social Rejection Impacts Subsequent Behavior.

Nelson, Brian Curtis

19 August 2009

It is proposed that differences in rejection attribution could yield variations in subsequent prosocial behavior. To test the attribution hypothesis, 109 participants were randomly assigned to a performance based rejection, a personally based rejection, or a control condition and then worked with an ostensible partner via the Internet to develop uses for a common household item. Prosocial behavior was measured by the number of uses a participant generated (working harder for the team). When generating creative uses, participants in the rejection conditions performed significantly worse than nonrejected participants (F(2,74) = 4.576, p<.05, r2=.11). However, in contradiction to the attribution hypothesis, participants in the 2 rejection conditions did not differ in performance. Explanations for why the rejection attribution hypothesis was not supported are discussed in addition to directions for future research regarding rejection attribution.

Social Rejection

Rejection Attribution

Attribution

Rejection

Psychology

Social and Behavioral Sciences

Social Psychology

Macrophage mediated endothelial injury and proliferation in renal transplant rejection

Adair, Anya

January 2008

Macrophages (Mφ) have previously been implicated in both acute and chronic renal allograft rejection however the mechanisms remain unclear. In this thesis I set out to explore the effect of the Mφ on the endothelium in the context of renal graft rejection. Initial studies focussed upon human renal allograft tissue from transplant nephrectomies performed because of chronic allograft nephropathy (CAN). Immunostaining was carried out on these tissues (n=29) and control kidney tissue obtained from nephrectomies performed for renal cell carcinoma (n=19). An increased interstitial Mφ infiltrate was found compared to control tissue. Immunostaining for the T cell marker CD3 and the B cell marker CD20 demonstrated that both lymphocyte populations were present in the CAN tissue with almost negligible numbers seen in control tissue. Previous work in the group had demonstrated a reduced number of CD31 positive peritubular capillaries in the tissues used in these studies. In the work undertaken in this thesis, additional analysis was performed to study lymphatic vessels. Immunostaining of control tissue with the lymphatic endothelial cell (LEC) marker podoplanin demonstrated a normal distribution of lymphatic vessels around large interlobular arteries. CAN tissue, however, exhibited an increased lymphatic density with lymphatic vessels evident within the interstitium; a finding verified with two additional LEC markers (LYVE-1 and VEGFR-3). Further investigations examined possible mediators that could be responsible for the reduced microvascular peritubular capillary network and increased lymphatic vessels present in tissues affected by CAN. Previous work had implicated nitric oxide (NO) generated by the enzyme inducible nitric oxide synthase (iNOS) in cardiac allograft rejection. Double immunolabelling for iNOS and the Mφ marker CD68 revealed evidence of Mφ expression of iNOS. No obvious reduction in vascular endothelial growth factor (VEGF)-A was evident although marked expression of VEGF-A was found in CD20 positive B cells within CAN tissue. Occasional interstitial cells expressed the lymphangiogenic growth factor VEGF-C, with double labelling studies indicating occasional CD68 +ve Mø that were positive for VEGF-C. In vitro studies were undertaken to dissect the interaction between Mø and microvascular endothelial cells (MCEC-1) using well established in vitro co-culture techniques. Co-culture of cytokine activated bone marrow derived Mø with MCEC-1 cells (a murine cardiac microvascular endothelial cell line) resulted in increasing levels of MCEC-1 apoptosis and a reduced cell number over a 24-hour time course. Non-activated Mø or cytokines alone were not cytotoxic. Co-cultures were performed in the presence of L-Nimino- ethyl lysine (L-Nil), a specific inhibitor of iNOS (control D-N6- (1-iminoethyl)-lysine (D-Nil)). L-Nil significantly inhibited MCEC-1 apoptosis and preserved cell number implicating a major role for NO in Mø-mediated MCEC-1 death. Importantly, L-Nil treatment did not affect TNFα production by cytokines suggesting that TNFα is not involved in MCEC-1 death in this in vitro experimental system. Experiments were then undertaken involving the depletion of Mø in a murine model of acute renal allograft rejection. Renal transplants were performed between donor Balb/c mice and either FVB/N CD11b-DTR mice transgenic for the diphtheria toxin receptor (DTR) under the CD11b promoter or control non-transgenic FVB/N mice. Diphtheria toxin (DT) was administered on days 3 and 5 to induce Mø depletion and mice sacrificed at day 7. Isograft controls were also performed between FVB/N mice. Murine allografts exhibited marked interstitial F4/80 positive Mø infiltration with expression of iNOS in the allografts. There was significant loss of peritubular capillaries (PTC) in allografts compared to isografts, indicating microvascular injury. DT treated CD11b-DTR mice exhibited 75% reduction in Mø infiltration and this was associated with dramatic microvascular protection. B and T cells were not evident in the isograft but significant accumulation of B and T cells was present in the allograft and not affect by Mø depletion. Interestingly, there was an increase in the number of podoplanin positive lymphatic vessels in the allograft compared to the isograft, which was significantly inhibited following Mø depletion. The final area of study focussed upon attempts to isolate lymphatic endothelial cells in vitro. Two types of vascular cells (HUVECs and HDMECs) were analysed by flow cytometry for LEC markers and immunofluorescence to phenotype the cells. Magnetic bead sorting was then undertaken to isolate discrete populations of endothelial cells expressing LEC markers. The murine studies reinforce the cytotoxic potential of Mø and supports a role for Mø in the deleterious rarefaction of microvascular interstitial vessels with resultant tissue hypoxia and ischaemia. Furthermore, these data support the involvement of Mø in the interstitial lymphangiogenesis that may occur in renal allografts. Furthermore, the study of human allograft tissue indicates that microvascular rarefaction and an increase in intrarenal lymphatic vessels occurs in human disease. Lastly, Mø expression of iNOS and VEGF-C suggests that Mø are involved in key processes that may adversely affect graft outcome.

616.079

99mTc labelling of interleukin-2 for in-vivo detection of lymphocytic infiltration

Chinaelli, Marco

January 1996

No description available.

610

Mechanisms in transplantation tolerance

Scully, Ralph

January 1994

No description available.

610

Complement regulation and xenotransplantation

Yannoutsos, Nikos

January 1996

No description available.

610.28

Role of the CD154-CD40 axis in the modulation of autoimmune reactions

Mars, Leonardus Theodorus

January 2000

No description available.

612

Diseases; Transplant rejection; T cells

Xenotransplantation : an investigation of cell-mediated rejection within a porcine xenograft model

Pleass, Henry

January 1995

No description available.

610

Rejection Sensitivity as Mediator Between Stigma and Romantic Relationship Satisfaction

Zangl, Jennifer

19 September 2013

HIV/AIDS is a highly stigmatizing condition that dramatically influences the social relations of those infected with the disease (Herek & Glunt, 1988; Kalichman, 2000). Stigmatized individuals experience interpersonal rejection because of their stigma and this rejection can heighten dispositional sensitivity to rejection (Downey & Feldman, 1996). Increased sensitivity to interpersonal rejection has been shown to decrease relationship satisfaction and lead to relationship dissolution (Downey, Freitas, Michaelis, & Khouri, 1998). Few studies have examined the influence of stigmatization on romantic relationships and little is known about the romantic relationships of people living with HIV/AIDS. The current study examined the role of rejection sensitivity as a mediator in the association between HIV/AIDS stigma and romantic relationship satisfaction. A diverse sample of HIV-positive participants was recruited from Vermont and neighboring states. Participants completed measures of perceived stigma, rejection sensitivity and satisfaction with their current romantic relationship. Disclosure concerns and enacted, or personalized, stigma predicted decreased relationship satisfaction. Rejection sensitivity did not mediate the relationship between stigma and relationship satisfaction. Results suggest that both rejection sensitivity and perceived stigma independently influence relationship satisfaction. The implications of the influence of stigma on romantic relationships are discussed.

HIV/AIDS

romantic relationships

rejection sensitivity

stigma