52 Main Points Robotic tubal reanastomosis is a safe, practical,

52 Main Points Robotic tubal reanastomosis is a safe, practical, and feasible method of fertility restoration in an appropriate selleck chem inhibitor patient population with pregnancy outcomes comparable with assisted reproductive technologies and surgical outcomes on par with laparoscopy. A robotic approach to adnexectomy is a feasible technique and may be associated with improved surgical outcomes (reduced intraoperative blood loss) in a subset of patients with a body mass index > 30. A robotic approach may be beneficial for the management of advanced stage IV endometriosis and conversion laparotomies to laparoscopies for more advanced cases. Compared with open surgery, robotic and laparoscopic approaches may be preferable in patients with type II ovarian debulking because of their significantly decreased postoperative complication rate.

Survival does not appear to be affected by surgical approach. The robotic approach to ovarian remnant syndrome management is associated with improved surgical outcomes but a lower rate of pain regression and increased incidence of adhesions and endometriosis compared with the laparoscopic approach. A robotic approach to cystectomy in the pediatric population may be a safe and feasible procedure with a low rate of complications and conversion to laparotomy. A robotic approach has been successfully applied in cases of ovarian transposition, ovarian vein syndrome, and salpingostomy for ectopic pregnancy.
Fetomaternal alloimmune thrombocytopenia (FMAIT) occurs when a woman becomes alloimmunized against fetal platelet antigens inherited from the fetus��s father (which are absent on maternal platelets), leading to fetal thrombocytopenia (< 150,000 platelets/��L).

Most cases are mild, with evidence of widespread petechiae and other skin lesions. However, severe cases can cause intracranial hemorrhage (ICH), resulting in death or long-term disability.1�C3 Unlike erythrocyte alloimmunization, FMAIT may appear during first pregnancies, with a high recurrence rate and often with progressively more severe manifestations in subsequent pregnancies.4�C6 FMAIT is the leading cause of severe thrombocytopenia in the newborn,7,8 and should not be confused with autoimmune thrombocytopenia, in which both mother and fetus are affected due to maternal autoantibodies. The prevalence of FMAIT has been variously reported as between 1 in 350 and 1 in 5000 live births.

5,7,9�C11 However, based on genetic probabilities,7,12 some authors believe that this entity is underdiagnosed and postulate a prevalence nearer to 1 in 1200 live births.10,13,14 At present, Batimastat there are no national screening programs for FMAIT and a history of an affected sibling is currently the best indicator of risk to a current pregnancy.15�C17 Etiopathogenesis FMAIT is produced by the placental transfer of maternal immunoglobulin (IgG) antibodies against fetal platelet antigens inherited from the father.

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