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Guidelines for laparoscopic treatment of ventral and incisional abdominal wall hernias (International Endohernia Society (IEHS)-part 1 [Guideline]

Bittner, R; Bingener-Casey, J; Dietz, U; Fabian, M; Ferzli, G S; Fortelny, R H; Kockerling, F; Kukleta, J; Leblanc, K; Lomanto, D; Misra, M C; Bansal, V K; Morales-Conde, S; Ramshaw, B; Reinpold, W; Rim, S; Rohr, M; Schrittwieser, R; Simon, Th; Smietanski, M; Stechemesser, B; Timoney, M; Chowbey, P
Guidelines are increasingly determining the decision process in day-to-day clinical work. Guidelines describe the current best possible standard in diagnostics and therapy. They should be developed by an international panel of experts, whereby alongside individual experience, above all, the results of comparative studies are decisive. According to the results of high-ranking scientific studies published in peer-reviewed journals, statements and recommendations are formulated, and these are graded strictly according to the criteria of evidence-based medicine. Guidelines can therefore be valuable in helping particularly the young surgeon in his or her day-to-day work to find the best decision for the patient when confronted with a wide and confusing range of options. However, even experienced surgeons benefit because by virtue of a heavy workload and commitment, they often find it difficult to keep up with the ever-increasing published literature. All guidelines require regular updating, usually every 3 years, in line with progress in the field. The current Guidelines focus on technique and perioperative management of laparoscopic ventral hernia repair and constitute the first comprehensive guidelines on this topic. In this issue of Surgical Endoscopy, the first part of the Guidelines is published including sections on basics, indication for surgery, perioperative management, and key points of technique. The next part (Part 2) of the Guidelines will address complications and comparisons between open and laparoscopic techniques. Part 3 will cover mesh technology, hernia prophylaxis, technique-related issues, new technologic developments, lumbar and other unusual hernias, and training/education.
PMCID:3872300
PMID: 24114513
ISSN: 1432-2218
CID: 1739572

A case of fatal fulminant myocarditis presenting as an acute ST-segment elevation myocardial infarction and persistent ventricular tachyarrhythmia associated with influenza A (H1N1) virus in a previously healthy pregnant woman

Ona, Mel A; Bashari, Daniel R; Tharayil, Zubin; Charlot, Aglae; Hoskins, Iffath; Timoney, Michael; Usmani, Shakeel; Royzman, Roman
Several studies have reported influenza A (H1N1) virus as a cause of fulminant myocarditis. We report the first fatal case of fulminant myocarditis presenting as an acute ST-segment elevation myocardial infarction and ventricular tachyarrhythmia associated with influenza A (H1N1) in a previously healthy pregnant woman. A 38-year-old Asian woman, gravida 3, para 1-0-1-1, presented with flu-like symptoms. Initially, she developed wide-complex tachycardia requiring several defibrillations and was later intubated. Electrocardiogram showed ST-segment elevation. Coronary angiogram was negative and a pulmonary angiogram ruled out pulmonary embolism. Fetal compromise was noted on the monitor, and the patient underwent an emergent cesarean section. She subsequently expired. Autopsy confirmed severe myocarditis. Further testing confirmed influenza A (H1N1) virus. This case of a rare, yet lethal, complication of H1N1 infection underscores the importance of increased awareness among health care professionals to provide pregnant women with vaccination and prompt treatment.
PMID: 23018755
ISSN: 0008-6312
CID: 248592

Innovative Approach to Treatment of the Metabolic Syndrome

Chapter by: Ricci, Joel; Timoney, Michael; Ferzli, George
in: Principles of metabolic surgery by Karcz, W; Thomusch, O [Eds]
Berlin ; New York : Springer, 2012
pp. 107-121
ISBN: 9783642024108
CID: 1772872

Guidelines for laparoscopic (TAPP) and endoscopic (TEP) treatment of inguinal hernia [International Endohernia Society (IEHS)] [Guideline]

Bittner, R; Arregui, M E; Bisgaard, T; Dudai, M; Ferzli, G S; Fitzgibbons, R J; Fortelny, R H; Klinge, U; Kockerling, F; Kuhry, E; Kukleta, J; Lomanto, D; Misra, M C; Montgomery, A; Morales-Conde, S; Reinpold, W; Rosenberg, J; Sauerland, S; Schug-Pass, C; Singh, K; Timoney, M; Weyhe, D; Chowbey, P
PMCID:3160575
PMID: 21751060
ISSN: 1432-2218
CID: 1739592

Impaired accessory cell function in a human dendritic cell line after human immunodeficiency virus infection

Beuria, Prarthana; Chen, Houchu; Timoney, Michael; Sperber, Kirk
We generated human dendritic cell (DC) hybridoma cell lines by fusing HGPRT-deficient promonocytic U937 cells with immature DCs obtained by culturing peripheral blood monocytes with interleukin-4 (IL-4; 1,000 U/ml) and granulocyte-macrophage colony-stimulating factor (100 U/ml) for 7 days and mature DCs by treatment with tumor necrosis factor alpha (12.5 microg/ml) for 3 days. Only one fusion with immature DCs was successful and yielded four cell lines--HB-1, HB-2, HB-3, and HB-9--with an overall fusion efficiency of 0.0015%. The cell lines were stable in long-term culture, displayed morphological features typical of DCs, and expressed distinct class I and class II molecules not present on U937 (A*031012, B*51011, Cw*0701, DRB3*01011 52, and DR5*01011). A representative cell line, HB-2, that expressed DC markers including CD83, CD80 and CD86 could be induced to produce IL-12 through CD40 stimulation. After human immunodeficiency virus (HIV) infection, there was impairment of antigen-presenting cell (APC) function, which was manifested by an inability to stimulate allogeneic T-cell responses. There was no change in expression of major histocompatibility complex class I and class II antigens, CD83, CD40, CD4, CD11c, CD80, CD86, CD54, and CD58, or IL-12 production in the HIV-infected HB-2 cells. The HIV-infected HB-2 cells induced T-cell apoptosis in the cocultures. T-cell proliferation could be partially restored by using ddI, indinivir, and blocking anti-gp120 and anti-IL-10 antibodies. Our data suggest that there are multiple mechanisms that DCs use to inhibit T-cell responses in HIV-infected patients. The HB-2 cell line could be a useful model system to study APC function in HIV-infected DCs.
PMCID:1065197
PMID: 15753259
ISSN: 1071-412x
CID: 1740622