Monday, October 21, 2019

Development of Inâ€Vitro Fertilization technology Essays

Development of In–Vitro Fertilization technology Essays Development of In–Vitro Fertilization technology Essay Development of In–Vitro Fertilization technology Essay 1. Introduction The pioneering work of Bob Edwards and Patrick Steptoe in the development of In Vitro Fertilization ( IVF ) engineering led to the first IVF birth of Louise Brown in 1978 [ I ] ( Johnson 2007 ) . It is considered one of the landmark parts to human medical specialty and wellness in the 20th century. In the last 20 old ages, there has been important advancement and scientific developments in the field of aided reproduction. The success rate of assisted generative engineering ( ART ) is continually increasing due to the debut of fresh engineerings, enhanced IVF techniques and improved embryo civilization systems [ two. The rapid gait of development in ART is besides straight linked to progresss in the clinical field of human reproduction and improved diagnosing of the causes of sterility. The field of ART will doubtless go on to turn in the following 20 old ages as there is a immense planetary demand for its medical and scientific advancement. More clinicians and scientists choose to come in this field every twelvemonth which is a testament to the success and turning importance of ART in medical specialty. 2. Sterility Infertility is defined as the lessened capacity to gestate or bear a kid ( Johnson 2007 ) . A twosome is considered sterile if they are unable to gestate after 2 old ages of unprotected and frequent sexual intercourse. The prevalence of sterility in the developed universe is estimated to be in the scope of 10s of female diseases and upsets doing sterility include: Tubal obstruction Endometriosis Polycystic Ovarian Syndrome Male factor sterility histories for approximately 30 % of the incidence of sterility. Examples of male diseases and upsets doing sterility include: Varicoceles Retrograde interjection Obstruction of vessel deferens or epididymis 30 % of incidence of sterility is due both male and female spouse have abnormalcies doing their sterility. The staying 20 % of infertile twosomes have no clinically identifiable cause for sterility and this group is termed unexplained sterility . The clinical work-up for sterility probe for any twosome includes documenting their medical history and a standard set of diagnostic trials to be performed on the male and female spouse ( Serhal A ; Overton 2004 ) for illustration: hormonal checks, hysterosalpingography, semen analysis. Establishing the cause of sterility allows clinicians to find which type of IVF intervention is the best to assist the twosome with gestating a kid. 3. Progresss in Infertility Treatment in the past 20 old ages The progresss in sterility intervention in the last 20 old ages are legion but I am merely discoursing the 1s which were of the most significance in my sentiment as follows. a. In- Vitro Fertilisation ( IVF ) The rule of the IVF technique is both simple and standard and can be summarised as follows [ four ] ( Strauss A ; Barbieri 2009 ) : Collection of mature oocytes from the ovaries Processing of seeds sample to better sperm count and motility Fertilization of sperm and oocyte in cell civilization dish in the research lab Transportation of embryo with best morphology into the uterine pit B. Controlled Ovarian Stimulation The female spouse undergoes a protocol of controlled ovarian stimulation. The pick of protocol is dependent on the age of the female spouse and the clinical diagnosing of sterility [ V ] ( Fauser et al 1999 ) . One of Steptoe and Edwards major job in their 1976 IVF process was the deficit of oocytes [ six ] ( Coughlan A ; Ledger 2008 ) . Surveies have shown that usage of ovarian stimulation protocols maximizes the figure and quality of mature follicles that can be retrieved [ seven ] ( Sluijmer 1994 ) [ viii ] ( Macklon et al 2008 ) which will necessarily better opportunities of IVF intervention success. In 1986, the add-on of Gonadotrophin Releasing Hormone ( GnRH ) agonist intervention to ovarian stimulation protocols became widespread [ nine ] ( Hedon et al 1990 ) . In the early 1990 s, ovarian stimulation protocols were refined with some fluctuations introduced in order to maximise the figure of eggs to be retrieved. The protocols used can be either: V Long OR Desensitization protocol: Starts with Pituitary receptor downregulation utilizing GnRH agonists e.g Lupron, Triptorelin, Burserelin Ovarian stimulation with GnRH injections of recombinant Follicle Stimulating Hormone ( FSH ) e.g Puregon Or Gonal F Injection of Human Chorionic Gonadotrophin ( HCG ) to command and clip oocyte ripening V Short OR Micro-Flare Protocol: GnRH antagonists e.g Cetrorelix Or Ganirelix are used to straight barricade the GnRH receptor. The undermentioned stairss are similar to Steps 2 A ; 3 of Long Protocol. Ovarian follicular growing is monitored by ultrasound imagination and measuring of blood degrees of oestradiol [ xi ] . The usage of GnRH adversaries has revolutionized ovarian stimulation for ART [ xii ] ( Ludwig et al 2001 ) . The Short Protocol was introduced in 1990 by [ xiii ] ( Bouchard et al. ) The advantages of the usage of GnRH adversaries in ART include: A more rapid IVF intervention rhythm Reduce the hazard of Ovarian Hyper-Stimulation Syndrome ( OHSS ) More effectual protocol for usage with older adult females and hapless respondents Avoids formation of ovarian cysts Cost effectual and more convenient for clinics and patients The usage of controlled ovarian stimulation is a major progress in IVF intervention and has contributed towards maximising success rates of clinical gestations and unrecorded births. There is no uncertainty that in the hereafter such protocols will be optimized and refined further for better clinical results. c. Oocyte retrieval In the 1st clinically successful IVF intervention, Bob Edwards and Patrick Steptoe retrieved the oocytes by laparoscopic surgery from the unstimulated ovaries of Louise s female parent during the natural catamenial rhythm [ xiv ] . The early 1980 s saw the development of high frequence vaginal investigation ultrasound transducers for usage in obstetric echography [ xv ] ( Lenz et al 1981 ) . In 1990, [ xvi ] ( Tan et al ) a survey outlined the advantages of utilizing vaginal ultrasounds for the process of oocyte retrieval. The process was termed Transvaginal Ultrasound Directed Oocyte Retrieval ( TUDOR ) and rapidly became the method of pick for usage in IVF clinics. The advantages of usage of TUDOR to laproscopic oocyte retrieval is that the latter is dearly-won and clip consuming. TUDOR can be done with local anesthesia and sedation which made it safer for patients and more convenient for IVF clinics ( Serhal A ; Overton 2004 ) . Laproscopic oocyte retrieval is performed presents merely in instances where female diseases such as adenomyosis or infective adhesions make the ovaries inaccessible through the transvaginal path. d. Testicular Sperm Extraction Male spouses with a clinical diagnosing of primary testicular failure will hold seeds analysis consequences bespeaking Low or No sperm count A ; motility. The development of testicular sperm extraction processs has provided such male patients with the possibility of recovering sperm for usage in IVF. The purpose of these processs is to assist the male patient to beget his ain familial kid. In 1995, Percutaneous Epididymal Sperm Aspiration ( PESA ) was a new process developed [ xvii ] ( Craft et al 1995 ) . It is a simpler and a more efficient process when compared to its predecessor Microscopic Epididymal Sperm Aspiration ( MESA ) which was developed in 1985 [ xviii ] . PESA is performed by infixing a suction needle into the caput of the epididymis and analyzing the aspirate for the presence of sperm [ xix ] In 1995, Testicular Sperm Extraction ( TESE ) was besides performed successfully in combination with IVF [ xx ] ( Devroey et al 1995 ) . The process involves taking a big fragment of testicular tissue through a cross scratch of the adventitia albuginea in the testicle [ xxi ] . Micro surgical TESE ( Micro-TESE ) is a polish to the TESE process. Numerous micro-retrievals of testicular tissue are performed across the testicle [ xxii ] ( Colpi et al 2009 ) . Micro-TESE has been associated with higher rates of sperm retrieval when compared to TESE ( Colpi et al 2009 ) . Aspirates incorporating sperm that are retrieved from the above stated processs can all be cryopreserved for subsequently usage in IVF. e. Intracytoplasmic Sperm Injection ( ICSI ) The micro-injection of a individual sperm into the cytol of the egg has revolutionized IVF intervention for twosomes with terrible male factor sterility [ xxiii ] ( Palermo et al 1992 ) . The technique is known as Intra Cytoplasmic Sperm Injection ( ICSI ) . Palermo et al reported the first successful ICSI gestation in 1992. Merely a little figure of sperms are equal for fertilisation utilizing ICSI which makes it an ideal process for male spouses with terrible male factor sterility following testicular sperm extraction processs. ICSI has enabled azoospermic male patients to beget their ain biological kids which was impossible in the past [ twenty-four ] ( Nijs A ; Elst 2000 ) . ICSI has become a mainstream process in ART. The chief stairss in ICSI technique can be summarised as follows: The oocyte is prepared by steadfastly attaching it to by suction to a keeping pipette with the polar organic structure at 6 oclock. A individual morphologically normal motile sperm is selected and immobilised. The injection acerate leaf is inserted into the oocyte at 3 oclock with careful deposition of the sperm into the cytol [ xxv ] ( Bromage et al 2007 ) . After 16 18 hours, fertilisation is confirmed by the presence of two pro-nuclei. ICSI is a technique that bypasses sperm oocyte adhering measure in the fertilization procedure and can therefore utilize sperm with lacking kinetic belongingss or anomalousnesss of the acrosome ( Palermo et al 1992 ) . Pregnancies and births have been reported after ICSI utilizing nonmotile sperm from ejaculate [ xxvi ] . ICSI still remains a controversial technique despite its world-wide clinical success in ART. The major concerns remain in the possible inauspicious results in kids born from this technique due to its invasive nature [ xxvii ] . The possible hazards of ICSI can attest in 3 general countries: Obstetric results: Low birth weight appears to be the most consistent hazard for ICSI kids [ twenty-eight ] ( Shieve et al 2002 ) Chromosomal Abnormalities: ICSI kids do transport an increased hazard of familial chromosomal aberrances. These are largely due to paternal Y chromosome microdeletions but can be due to maternal familial factors every bit good [ xxix ] ( Rubio et al 2001 ) . There is an increased hazard of forming upsets [ thirty ] ( Cox et al 2002 ) e.g Angelman Syndrome. These surveies emphasize the importance of familial guidance to IVF twosomes prior to ICSI. Developmental Abnormalities: No major developmental abnormalcies are observed nevertheless some surveies have reported lower mental development rate in ICSI kids when compared to IVF and natural construct rhythms [ thirty-one ] ( Bowen et al 1998 ) The mechanical harm done to the oocyte and its meiotic spindle during ICSI technique and the possible transportation of sperm mitochondrial Deoxyribonucleic acid into the oocyte are besides major countries of concern with ICSI. Sperm choice during ICSI is non natural and relies on opinion of the clinical embryologist. The PICSI sperm choice device was developed in 2006 to better the effectivity and cut down hazards of unreal sperm choice during ICSI. Sperm are placed in PICSI dish which contains samples of hyaluronan hydrogel which mimics the natural hyaluronan bed environing the oocyte [ xxxii ] ( ESHRE 2006 ) . Merely those that bind to the hyaluronan microdots mimic natural sperm choice procedure and are selected for ICSI. A survey completed in 2009 to measure the efficaciousness of PICSI + ICSI versus ICSI entirely, found that the clinical gestation rate in the PICSI group was greater by 6 % when compared to the ICSI entirely group [ xxxiii ] ( Worrilow et al 2009 ) f. Assisted Embryo Hatching Hatch of the human embryo from its environing Zona Pellucida is a cardinal demand for its successful nidation in the receptive endometrium ( Johnson 2007 ) . Failure of embryo hatching can restrict the nidation rate which will impact IVF intervention success. Zona Pellucida hardening can be induced by the in vitro civilization conditions and increased maternal age [ xxxiv ] ( Cohen et al 1990 ) . Assisted Hatching ( AH ) of embryos was started in the early 90 s when surveies showed betterment in nidation rates ( Cohen et al 1990 ) . AH is by and large performed on twenty-four hours 3 post-fertilization. It is a micromanipulation technique performed automatically by boring an gap in the Zona or by chemically thinning it by utilizing an acidified solution [ xxxv ] ( Chao et al 1997 ) . From the twelvemonth 2000 onwards, surveies have reported on the efficaciousness of Laser assisted hatching ( LAH ) [ thirty-six ] ( Hseih et al 2002 ) . The impact of LAH remains controversial due to fear of its mutagenic consequence on the embryo, but several surveies conclude that better clinical results are achieved with LAH when compared to the mechanical techniques, in adult females of advanced age ( gt ; 37 old ages ) and with insistent IVF failure [ xxxvii ] ( Makrakis et al 2006 ) [ xxxviii ] ( Ali et al 2002 ) . However, there is still non adequate grounds to reason which AH method is superior to the others. The major hazards associated with AH technique include: Increased hazard of monozygotic twins Damage to the embryo and its single blastomeres Introduction of micro-organisms into the embryo through the zone hole. g. Preimplantation Genetic Diagnosis Preimplantation Genetic Diagnosis ( PGD ) is a specialised process that was developed for twosomes who are at hazard of conveying a known familial disease to their kids. The alternate intervention options available for these twosomes include: expiration of gestation if antenatal diagnosing confirms an affected foetus, gamete contribution through IVF or acceptance [ xli ] . In 1990, [ xlii ] Handyside et Al reported the first human gestation following usage of PGD in two twosomes at hazard of conveying adrenoleukodystrophy and X-linked mental deceleration. PGD involves three phases: Use of IVF: to make embryos Embryo biopsy: There are 3 methods presently being used: Polar Body Biopsy: remotion of 1st and 2nd polar organic structure Blastocyst Biopsy: remotion of some trophectoderm cells Cleavage Phase Biopsy: Is the most common method used and involves remotion of 1 2 blastomeres from 6 8 cell embryo [ xliii ] ( Harper 2009 ) . Single Cell Diagnosis: Cells extracted after biopsy are tested by: Polymerase Chain Reaction ( PCR ) : for diagnosing of individual cistron defects ( e.g Cystic Fibrosis ) , X Linked Diseases ( e.g Haemophilia ) and Triplet Repeat Disorders ( e.g Myotonic Dystrophy ) Fluorescent In Situ Hybridization ( FISH ) : for analysis of chromosomal abnormalcies [ xliv ] Even though PGD is an invasive and expensive process it offers twosomes a curative birthrate intervention that prevents the transmittal of their familial disease. Recently the applications of PGD have been extended to name for familial malignant neoplastic disease sensitivities [ forty-five ] ( Spits et al 2007 ) and for human leucocyte antigen ( HLA ) matched offspring to bring forth a healthy kid that is indistinguishable to his / her affected sibling [ xlvi ] ( Verlinsky et al 2001 ) besides known as saviour sibling . Sexual activity choice for societal grounds can besides be performed by PGD nevertheless this remains a extremely controversial application [ xlvii ] ( Shenfield et al 2003 ) . The field of PGD is quickly germinating and this has led to moral A ; ethical concerns over its practical application for non-medical grounds. h. Cryopreservation of Embryos Embryo cryopreservation is an of import concluding measure in IVF intervention. Cryopreservation of trim embryos involves puting them in cryoprotectant solution and hive awaying them in liquid N. Embryo cryopreservation reduces the demand for multiple embryo transportations during an IVF rhythm as trim healthy embryos can be stored successfully ( Serhal A ; Overton 2004 ) . This finally helps cut down the multiple gestation hazard associated with IVF intervention. Slow freeze has been the primary method for cryopreservation in the 80 s and the first human gestation from frozen embryo was in 1983 [ xlviii ] ( Trounson A ; Mohr 1983 ) . However, slow freeze is associated with ice crystal formation, cell lysis and blastomere flight peculiarly in PGD biopsied embryos [ xlix ] ( Magli et al 1999 ) . In 2000, a new alternate method termed for cryopreservation of human embryos was introduced with a rapid freeze protocol [ cubic decimeter ] ( Saito et al 2000 ) . Vitrfication is a procedure by which liquid turns into solid without the formation of ice crystals [ fifty-one ] ( Luyet A ; Hodapp 1938 ) . The vitrification protocol quickly revolutionized both embryo and gamete ( peculiarly oocyte ) cryopreservation. It is a low-priced and efficient method that can be performed at cleavage, morula A ; blastocyst phase [ lii ] ( Kuwayama et al 2005 ) . It consequences in decreased ice crystal formation and lower DNA harm to blastomeres following zonary h atching [ liii ] ( Kader et al 2007 ) . Vitrification significantly improved station melt endurance rates, embryo development and gestation rates [ fifty-four ] ( Kolibianakis et al 2009 ) . One issue of concern raised with vitrification protocol is the direct contact between embryos and liquid N [ lv ] ( Huang et al 2007 ) . This raises concern of possible bacterial A ; viral cross-contamination peculiarly in biopsied embryos [ lvi ] ( Bielanski et al 2000 ) nevertheless a possible solution would be to hive away the embryos in vapour stage of liquid N [ lvii ] ( Cobo et al 2007 ) . There is no uncertainty that farther alterations and betterments to current vitrification protocol will be introduced in the hereafter to farther optimise embryo cryopreservation processs. 3. What will the following 20 old ages bring for sterility intervention? The legion developments and success rates of IVF intervention has so far likely exceeded the outlooks of Edward and Steptoe themselves. The hereafter will convey betterments to the current techniques mentioned in old subdivision as optimisation of protocols is linked to progresss in engineering and scientific research. The following 20 old ages will perchance keep another exciting chapter in ART. a. Artificial Gametes Patients who wish to undergo IVF intervention but have absent or non feasible gametes are presently non being offered ART with the chance of bring forthing their biological progeny. The alternate intervention to such twosomes would be gamete contribution coupled with conventional IVF. The figure of twosomes seeking gamete contribution is increasing and this is partially due to detain kid bearing age in modern society. This presents a challenge to the hereafter of sterility intervention. Recent surveies have shown that mouse embryologic root cells ( ESC ) can distinguish into sperm [ lviii ] ( Geijsen et al. 2004 ) and oocytes [ lix ] ( Hubner et al.2003 ) . Another survey concluded that human ESCs can besides distinguish into germ cells in civilization [ sixty ] ( Clark et al. 2004 ) . The creative activity of unreal gametes involves bodily cell atomic transportation ( SCNT ) of a diploid karyon into the cytol of an enucleated oocyte with the purpose of bring forthing a cloned embryo [ lxi ] ( Nagy A ; Chang 2008 ) . ESCs derived from the cloned embryo can be differentiated in vitro into monoploid sperm and oocytes [ lxii ] ( Zubin 2006 ) . Customized gametes of the opposite sex can besides be created utilizing SCNT from a male karyon as it possesses both X and Y chromosomes nevertheless this is more hard for a female karyon as it can non distinguish into sperm as it does nt possess Y-chromosome cistrons. Further research is required to measure the possible hazards of ESC gamete creative activity in ART and its medical A ; ethical deductions. Surveies have shown that micromanipulation of cells during SCNT can bring on forming and epigenetic mutants [ sixty-three ] ( Humphreys et al 2002 ) every bit good as neglecting to trip cardinal embryologic cistrons [ sixty-four ] ( Bortvin et al 2003 ) . This is both an expensive and labour intensive procedure and farther research is required to do it an efficient A ; safe procedure for its hereafter usage in sterility intervention. Scientific research in this field is assuring A ; will doubtless come on further in the following 20 old ages. Artificial gametes can be used by twosomes who have spiritual expostulations to utilizing donor gametes or who wish to hold genetically indistinguishable kids. Customized gametes can besides be used by same sex twosomes and this offers them picks in ART. B. Designer Babies The rapid progresss in the field human genetic sciences and completion of the human genome undertaking has improved familial alteration engineering and its application in medical specialty. Scientific research is continuously set uping familial links with common diseases. Future progresss in IVF intervention can increase the easiness and efficiency of the PGD procedure. This will take to farther mainstream usage of ART for non medical grounds. PGD offers the engineering for increased familial generative pick to parents. In the following 20 old ages IVF coupled with PGD can be used to: transportation gender selected embryos transportation embryos absent of cistrons for less life threatening diseases e.g diabetes, high blood pressure, adenomyosis transportation embryos with selected non medical traits e.g height, hair A ; oculus coloring material and intelligence. The term Designer Babies is tricky but is deceptive because multi-factorial familial traits are influenced by environmental factors and besides PGD choice is limited to the cistron pool of the parents [ sixty-five ] ( Toukhy A ; Braude 2008 ) . The hereafter of PGD remains controversial and applications of the technique will be capable to more legal and ethical argument. The following 20 old ages may besides present familial sweetening of embryos by changing their familial makeup as chosen by parents. This is non executable with current engineering but future scientific developments may do it possible for usage in ART. c. Embryo Screening The progresss in IVF intervention have still non been able to extinguish its major hazard. Almost a 3rd of IVF gestations involve multiple gestations ( Coughlan A ; Ledger 2008 ) . Multiple births are associated with increased morbidity A ; mortality [ lxvi ] ( Hardy et al 2002 ) . Twin A ; three gestations are common in IVF and are a consequence of the transportation of more than one embryo in the receptive endometrium. This is done peculiarly for female patients with advanced maternal age ( gt ; 35 old ages ) and hapless forecast and this represents a big cohort of IVF patients. The following 20 old ages may convey developments to the undermentioned methods: Optimize the civilization media for human embryos: The challenge will be to alter the alimentary concentration of the civilization media to seek and mime every bit much as possible the in vivo environment of the fallopian tubing. This will better embryo development prior to reassign. Improve embryo scaling and choice: Embryo are selected harmonizing to their morphology and developmental rate. This is non the best method for choosing feasible embryos. Hopes for drawn-out embryo culturing in the hereafter may let further development of embryos, after the blastodermic vessicle phase, to better choice of healthy embryos. Aneuploidy Screening: Designation of chromosomal abnormalcies in embryos of older IVF patients is an of import showing tool to avoid nidation failure [ lxvii ] ( Fragouli et al 2006 ) . Comparative genomic Hybridisation ( CGH ) is a promising technique that allows efficient sensing of chromosomal aneuploidies in one experiment utilizing individual blastomeres or polar organic structures [ sixty-eight ] ( Wells et al 2002 ) . The following 20 old ages will convey optimisation of a rapid A ; cheap CGH protocol which will greatly progress whole genome embryo testing techniques in antenatal nosologies. Mentions: Johnson M. H. ( 2007 ) . Essential Reproduction, 6th erectile dysfunction: Wiley-Blackwell.Pg 299 Serhal P. A ; Overton C. ( 2004 ) .Good Clinical Practice in Assisted Reproduction, Cambridge University Press Heffner L. J. and Schust D. J. ( 2010 ) .The Generative System at a Glance, 3rd Ed. Wiley Blackwell Strauss J. A ; Barbieri R. ( 2009 ) Yen A ; Jaffe s Reproductive Endocrinology, 6th Ed, Elsevier. Ch 29, Pg 725-757 Fauser B.C. , Devroey P. , Yen S.S, Minimal ovarian stimulation for IVF, assessment for potency for benefits and drawbacks, Human Reproduction ( 1999 ) , Vol 14, pp. 2681-2686 Coughlan C. A ; Ledger W. , In Vitro Fertilisation. ( 2008 ) , Obstetrics, Gynaecology A ; Reproductive Medicine, Vol 18: Issue 11 Sluijmer A.V. , Effect of pituitary down-regulation on the ovary before in vitro fertilisation as measured utilizing 3-dimensional power Doppler ultrasound ( 1994 ) Birthrate and Sterility, Vol 79: Issue 5, pp 1129-1135 Macklon N. S, Van der Gaast M. H, Hamilton A, Fauser B, Giudice L, The Impact of Ovarian Stimulation With Recombinant FSH in Combination With GnRH Antagonist on the Endometrial Transcriptome in the Window of Implantation, ( 2008 ) Reproductive Sciences, Vol15: Issue 4, pp 357-365 Hedon B, Bringer J, Arnal F, Humeau C, Boulot P, Audibert F, Benos P, Neveu S, Mares P, Laffargue F, Viala J. L, The usage of GnRH agonists with hMG for initiation or stimulation of ovulation ( 1990 ) Bailli A ; egrave ; rhenium s Clinical Obstetricss and Gynaecology, Vol 4: Issue 3, pp 575-587 Tarlatzis B.C. A ; Kolibianakis E.M, GnRH Agonists VS Antagonists ( 2007 ) Best Practice A ; Research Clinical Obstetrics A ; Gynaecology, Vol 21: Issue 1, pp 57-65 Felberbaum R.E, Ludwig M, Diedrich K, Clinical application of GnRH Antagonists ( 2000 ) , Molecular Cellular Endocrinology Vol 166 pp. 9-14 Ludwig M, Katalinic A, Diedrich K, Use of GnRH adversaries in ovarian stimulation for aided generative engineerings compared to the long protocol ( 2001 ) Archives of Gynecology and Obstetrics Vol 265 pp 175-182 Bouchard, P. , Caraty, A. and Medalie, D. Mechanism of action and clinical utilizations of GnRH adversaries in adult females. ( 1990 ) Recent Progress on GnRH and Gonadal Peptide ; Elsevier Edwards R.G. , The bumpy route to human in vitro fertilization, ( 2001 ) , Nature Medicine Vol 7 pp. 1091-1094 Lenz. S. , Lauritsen J.G. , Kjellow, M. Collection of human oocytes for in vitro fertilisation by ultrasonically guided follicular pucture. ( 1981 ) Lancet, Vol I, pp 1163-4 Tan S.L. , Bennett S. , Parsons J. Surgical techniques of oocyte aggregation and embryo transportation ( 1990 ) British Medical Bulletin, Vol 46 pp 628 42 Trade I, Tsirigotis M, Bennett V, Taranissi M, Khalifa Y, Hogewind G, et Al. : Transdermal epididymal sperm aspiration and intracytoplasmic sperm injection in the direction of sterility due to clogging azoospermia. ( 1995 ) Fertility A ; Sterility, Vol 63, pp 1038-42. Temple-Smith PD, Southwick GJ, Yates CA, Trounson AO, de Kretser DM: Human gestation by in vitro fertilisation ( IVF ) utilizing sperm aspirated from the epididymis. ( 1985 ) Journal of In Vitro Fertilization A ; Embryo Transfer, Vol 2 pp 119-22. Glina S. , Fragoso J. B, Martins F.G, Soares J.B, Galuppo A.G. PERCUTANEOUS EPIDIDYMAL SPERM ASPIRATION ( PESA ) IN MEN WITH OBSTRUCTIVE AZOOSPERMIA ( 2003 ) International Brazilian Journal of Urology, Vol 29 pp 141-146. Devroey, P. , Liu, J. , Nagy Z. , Goosens, A. , Tournaye, H. , Camus, M. , Van Steirteghem, A. and Silber, S. Pregnancies after testicular sperm extraction and intracytoplasmic sperm injection in non-obstructive azoospermia ( 1995 ) , Human Reproduction, Vol 10, pp 1457-1460. Colpi G.M. , Colpi E.M. , Piediferro G. , Giacchetta D. et Al, Microsurgical TESE versus conventional TESE for ICSI in non-obstructive azoospermia: a randomized controlled survey ( 2009 ) , Reproductive Bio Medicine Online, Vol 18, pp 315 319 Pantke P. , Diemer T. , Marconi M. , Bergmann M. , Steger K. , Schuppe H.C, Weidner W.Testicular Sperm Retrieval in Azoospermic Men. ( 2008 ) , European Urology Vol 7, pp 703 -14 G Palermo, H Joris, P Devroey and AC Van Steirteghem, Pregnancies after Intracytoplasmic injection of individual sperm cell into an oocyte ( 1992 ) , Lancet Vol 340 pp. 17-18 Nijs M. A ; Elst H. , Biological facets of testicular sperm extraction. ( 2000 ) , European Journal of Obstetrics A ; Gynecology and Reproductive Biology, Vol 92, pp 1 6 Bromage S.J. , Falconer D.A. , Lieberman B. , Sanger V. , Payne S. , Sperm Retrieval Rates in Subgroups of Primary Azoospermic Males. ( 2007 ) , European Urology, Vol 51, pp 534-540 Barros A, Sousa M, Oliveira C, Silva J, Almeida V, Beires J. Pregnancy and birth after intracytoplasmic sperm injection with wholly nonmotile sperm recovered from the semen. ( 1997 ) Birthrate and Sterility, Vol 67: Issue 6, pp 1091-1094 Matthew G. Retzloff M.D. , Hornstein D. , Is intracytoplasmic sperm injection safe? ( 2003 ) , Fertility and Sterility, Vol 80: Issue 4, pp 851-859 Schieve L. , Meikle S. , Ferre C. , Petersen H. , Jeng G. , Wilcox L. , Low and really low birth weight in babies conceived with usage of aided generative engineering. ( 2002 ) , New England Journal of Medine Vol 346, pp. 731-737. Rubio C. , Gil-Salom M. , Simon C. , Vidal F. , Rodrigo L. , Minguez Y. et al. , Incidence of sperm chromosomal abnormalcies in a hazard population: relationship with sperm quality and ICSI result. ( 2001 ) , Human Reproduction Vol 16, pp. 2084-2092. Cox G. F. , Burger J. , Lip V. , Mau U.A. , Sperling K. , Wu B.L. et al. , Intracytoplasmic sperm injection may increase the hazard of forming defects, ( 2002 ) , American Journal of Human Genetics, Vol 71, pp. 162-164. Bowen J. R. , Gibson F.Z. , Leslie G. I. , Saunders D.M. , Medical and developmental result of 1 twelvemonth for kids conceived by intracytoplasmic sperm injection. ( 1998 ) Lancet, Vol 351, pp. 1529-1534. ESHRE Meeting Prague, CZ. June 17, 2006 Biocoat, Inc. Announces FDA Marketing Clearance for Its New PICSIÂ ® Sperm Selection Device ; www.midatlanticdiagnostics.com Worrilow, S. Eid, J.M. Matthews, E.J. Pelts, C. Khoury and J. Liebermann. A multi-site clinical test measuring PICSIÂ ® versus intracytoplasmic sperm injection ( ICSI ) : positive clinical results observed in a prospective, randomised and double-blinded survey. ( 2009 ) Birthrate and Sterility, Vol 92: Issue 3, pp S36-S37 Cohen J. , Elsner C. , Kort H. , Malter H. , Massey J. , Mayer M.P et al. , Impairment of hatching procedure following IVF in the human and betterment of nidation by aided hatching utilizing micromanipulation. ( 1990 ) , Human Reproduction, Vol 5, pp. 7-13. Chao K.H. , Chen S. U. , Chen H.F. ,

No comments:

Post a Comment

Note: Only a member of this blog may post a comment.