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Background
Lyssencephaly Smoothbrain (froomtheGreek“lissos” and “enkhapalos”) Cerebral cortexscarces of: Gyri Groove Fissures
Malformation of thephysicalstructureisbecauseitdidn’tdevelopedcompletelywhileembryonicdevelopment. Lack of embryonicdevelopment: Low blood flow CongenicCitomegalovirus (cCMV) Genetic mutation (LIS1, XLIS)
Researches Malformations of cortical development in children with congenital cytomegalovirus infection - A study of nine children with proven congenital cytomegalovirus infection  Development of Lissencephaly in the fetus as direct consequence of early infection. Most common vertically transmitted disease  rate of the infection ranging:  0.2 to 2.4% in newborn infants 40.000 infants per year
Chemical remedy Oral Hexadecyloxypropyl-Cidofovir Therapy in Pregnant Guinea Pigs Improves Outcome in the Congenital Model of Cytomegalovirus Infection Alternative orally supply analog of the existing drug, Cidofovir Only proved effiency of Guinea Pigs
Why supply antibodies?
Hypothesis 	The augment of antibodies IgG and IgM may reduce the presence of CVM, representing a minor risk to the fetus in developing Lissencephaly.
Objectives ,[object Object]
Reduce the CMV presence in the placenta
Lower the risks of developing Lissencephaly caused by cCMV.,[object Object]
Materials CMV Pp38 (UL80a), Cytomegalovirus Antigen, Recombinant IgMAntibody, mAb, Mouse Mouse IgG control (Whole Molecule), Purified IL-4 Antibody (2G6A8), mAb, Mouse Mouse IL-28A/B  39female pregnant MusMusculus Image Cytometri
Light diagnostics CMV direct Immunofluorescence Assay Kit Dextran Leukocyte Separation Kit Formaldehyde-NoidetP-40 MRI
Methodology
Step: Prepare research models
Prepare research models Mice from 12-13 days Anesthiaze mice Inject with CMV vector solution with a glass micropipette Place pipette for an 30 s and then slowly withdrawn.
Research model’s distribution Groups: IL 6 IL 28 IgG IgM Sub-groups: A= every week B= every 48 hrs C= every three days
Step: Viral presence assays
Extract serology: CVS Placenta is the common path  Chronic Villous Sampling Suction of a tissue from placenta
Step: ELISPOT Quantify presence of IgG and IgM in all experimental groups Procedure according to: “General ELISPOT procedure” by abcam.com
Step: Direct immunofluorescence Cualitative presence of IgG and IgM in all experimental groups Process according to: “Immunostaining of cells in tissue culture” by ENCORE biotechnology INC.
Spected results ELISPOT will indicate:  augment in antibodies in experimental groups will mean lower presence of CMV Direct immunofluorescence: Control group will be brighter than experimental groups will mean high presence of CMV
Bibliography  Bosnjak VM, Daković I, et al. Malformations of cortical development in children with congenital cytomegalovirus infection - A study of nine children with proven congenital cytomegalovirus infection. January, 2011. http://www.ncbi.nlm.nih.gov/pubmed/21648339 Ravo FJ, Bernstein DI, et al. Oral Hexadecyloxypropyl-Cidofovir Therapy in Pregnant Guinea Pigs Improves Outcome in the Congenital Model of Cytomegalovirus Infection. November 15, 2011. http://www.ncbi.nlm.nih.gov/pubmed?term=Oral%20Hexadecyloxypropyl-Cidofovir%20Therapy%20in%20Pregnant%20Guinea%20Pigs%20Improves%20Outcome%20in%20the%20Congenital%20Model%20of%20Cytomegalovirus%20Infection%20

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Proposal

  • 2. Lyssencephaly Smoothbrain (froomtheGreek“lissos” and “enkhapalos”) Cerebral cortexscarces of: Gyri Groove Fissures
  • 3. Malformation of thephysicalstructureisbecauseitdidn’tdevelopedcompletelywhileembryonicdevelopment. Lack of embryonicdevelopment: Low blood flow CongenicCitomegalovirus (cCMV) Genetic mutation (LIS1, XLIS)
  • 4. Researches Malformations of cortical development in children with congenital cytomegalovirus infection - A study of nine children with proven congenital cytomegalovirus infection Development of Lissencephaly in the fetus as direct consequence of early infection. Most common vertically transmitted disease rate of the infection ranging: 0.2 to 2.4% in newborn infants 40.000 infants per year
  • 5. Chemical remedy Oral Hexadecyloxypropyl-Cidofovir Therapy in Pregnant Guinea Pigs Improves Outcome in the Congenital Model of Cytomegalovirus Infection Alternative orally supply analog of the existing drug, Cidofovir Only proved effiency of Guinea Pigs
  • 7. Hypothesis The augment of antibodies IgG and IgM may reduce the presence of CVM, representing a minor risk to the fetus in developing Lissencephaly.
  • 8.
  • 9. Reduce the CMV presence in the placenta
  • 10.
  • 11. Materials CMV Pp38 (UL80a), Cytomegalovirus Antigen, Recombinant IgMAntibody, mAb, Mouse Mouse IgG control (Whole Molecule), Purified IL-4 Antibody (2G6A8), mAb, Mouse Mouse IL-28A/B 39female pregnant MusMusculus Image Cytometri
  • 12. Light diagnostics CMV direct Immunofluorescence Assay Kit Dextran Leukocyte Separation Kit Formaldehyde-NoidetP-40 MRI
  • 15. Prepare research models Mice from 12-13 days Anesthiaze mice Inject with CMV vector solution with a glass micropipette Place pipette for an 30 s and then slowly withdrawn.
  • 16. Research model’s distribution Groups: IL 6 IL 28 IgG IgM Sub-groups: A= every week B= every 48 hrs C= every three days
  • 18. Extract serology: CVS Placenta is the common path Chronic Villous Sampling Suction of a tissue from placenta
  • 19. Step: ELISPOT Quantify presence of IgG and IgM in all experimental groups Procedure according to: “General ELISPOT procedure” by abcam.com
  • 20. Step: Direct immunofluorescence Cualitative presence of IgG and IgM in all experimental groups Process according to: “Immunostaining of cells in tissue culture” by ENCORE biotechnology INC.
  • 21. Spected results ELISPOT will indicate: augment in antibodies in experimental groups will mean lower presence of CMV Direct immunofluorescence: Control group will be brighter than experimental groups will mean high presence of CMV
  • 22. Bibliography Bosnjak VM, Daković I, et al. Malformations of cortical development in children with congenital cytomegalovirus infection - A study of nine children with proven congenital cytomegalovirus infection. January, 2011. http://www.ncbi.nlm.nih.gov/pubmed/21648339 Ravo FJ, Bernstein DI, et al. Oral Hexadecyloxypropyl-Cidofovir Therapy in Pregnant Guinea Pigs Improves Outcome in the Congenital Model of Cytomegalovirus Infection. November 15, 2011. http://www.ncbi.nlm.nih.gov/pubmed?term=Oral%20Hexadecyloxypropyl-Cidofovir%20Therapy%20in%20Pregnant%20Guinea%20Pigs%20Improves%20Outcome%20in%20the%20Congenital%20Model%20of%20Cytomegalovirus%20Infection%20
  • 23. Araswathy TS, Az-Ulhusna A, et al. Seroprevalence of cytomegalovirus infection in pregnant women and associated role in obstetric complications: a preliminary study. March, 2011. http://www.ncbi.nlm.nih.gov/pubmed/21710852 Kaneda K, Kasahara H, et al.Selective Optical Control of Synaptic Transmission in the Subcortical Visual Pathway by Activation of Viral Vector-Expressed Halorhodopsin. April 5, 2011. http://www.ncbi.nlm.nih.gov/pubmed?term=Selective%20Optical%20Control%20of%20Synaptic%20Transmission%20in%20the%20Subcortical%20Visual%20Pathway%20by%20Activation%20of%20Viral%20Vector-Expressed%20Halorhodopsin Boeckh, M. and Boivin, G. Quantitation of Cytomegalovirus: Methodologic Aspects and Clinical Applications. Clinical Microbiology Reviews, July 1998, p. 533-554, Vol. 11, No. 3. http://cmr.asm.org/cgi/content/full/11/3/533

Editor's Notes

  1. Researches as Malformations of cortical development in children with congenital cytomegalovirus infection - A study of nine children with proven congenital cytomegalovirus infection affirm that... “Congenital cytomegalovirus (CMV) infection is the most common vertically transmitted disease with the rate of the infection ranging from 0.2 to 2.4% in newborn infants”.
  2. A chemical remedy had already been experimented inOral Hexadecyloxypropyl-Cidofovir Therapy in Pregnant Guinea Pigs Improves Outcome in the Congenital Model of Cytomegalovirus Infectionas an alternative orally supply analog of the existing drug, Cidofovir, against CMV
  3. 125 pregnant women tested, IgG antibody was found 84% (105 women) of the times, but IgM only on 7.2% (9 women)It means that they weren’t always present, signifying lack of antibody levels. Therefore, that can be reasoned that... (hypothesis)
  4. Musmusculus, because:resemblance to human, able to be infected with CMV, more ethical to work with than humans, small sized, highly fertile, principally because isgraded as ideal for ‘in vivo’ hybridomasto produce continuous supply of antibody. Division:9 for each experimental group + 3 for the control group.Image Citometri = stores image data and the microscopic parameters describing the optics during the acquisition.
  5. Dextran Leukocyte Separation Kit = isolation of the PMN by dextran separation PMN Polymorphonuclear leukocytes:CMV DNA can be detected in different fractions of leukocytes like this one during active infectionFormaldehyde-Noidet P-40=solution made of a simple Aldehyde and a detergent.MRI= Magnetic Resonance Image
  6. Selective Optical Control of Synaptic Transmission in the Subcortical Visual Pathway by Activation of Viral Vector-Expressed Halorhodopsin.Anestethiaze with ketamineand xylazineInject mice with unilateral pressure injections of 1.0–1.5 µl of CMV vector solution (Recombinant CMV) into the body using a glass micropipette with a tip diameter of 20–30 µm.Place pipette for an 30 s and then slowly withdrawn.  
  7. IL 6 =B-cell stimulatory factorIL 28=inmune defense against virusIgG=  battle bacterial and viral infectionsIgM= first reponse against antigen presenceEach will be for a complete of period fifteen days, because the sampling can be made days before the offspring born.
  8. After fifteen days of gestation, the CVS (Chronic Villous Sampling) in order to analyze the placenta tissue. Placenta is the organ where the mother supplies the fetus important needs for the development as nutritional and respiratory.