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L/O/G/O
A thesis Submitted in Partial Fulfillment of the Requirements for (M.D.) in
Obstetrics & Gynecology By Moataz Gamal Taha Abu-Shahba (2014)
Specialist of Obstetrics &Gynecology Al-Galaa Teaching Hospital
• Praise be to Allah, who exalted in knowledge
whom he wills; but above those that have
knowledge, there is one more knowing; to
Him is the goal and to Him is the return of all.
• Supervising Professors
Especially Professor Fawzy Abel Aziz,
Professor Mohamed Sherif El-Sayes and
Dr. Mohamed Ibrahim Mostafa
• My Family (Mother, brothers, wife, children).
Acknowledgments
INTRODUCTION
Preterm labor
 Birth of a baby of less than 37 weeks gestational age.
 The cause is elusive and unknown.
 The reduction of PTL is a challenging proposition.
 PTB vs. premature birth.
 PTB is among the top causes of death in infants
worldwide.
Epidemiology & Magnitude of The Problem
 In Europe, PTB is generally 5-9% and in USA it has been
risen to 12-13% in the last decades.(Goldenberg,2008).
 It is estimated that one-third of LBW deliveries are due to
preterm delivery.
 PTB is a significant cost factor in healthcare including long
term care for disabilities .
 550.000 PTB each year in USA , run up 26$ billion ,
mostly related to NICU.
Etiology (Risk
F.)
Diagnosis
Symptoms
signs
Initial
Evaluation
• Gestational age
• ROM
• Infection
• In Labor
• T/V U/S&/or FFN
Assess
ROM
• Speculum ex. (sample for FFN, ,
alkalinity, nitrazine paper test
Assess for
infection
• Urine sample(bacteriuria, &P.N.)
• RectoVaginal culture(GBS)
• Gonorrhea,B.V.,&T.V.
Diagnosis
True labor
• Regular Uterine contra.+dilat. &effeac. +descent
(3cm,80%,ROM& V.Bl.)
FFN
• -ve predictive value 99%
• +ve predictive value 13-30%
Aminosure® • One step immuno chromatographic assay.(PAMG-1)
T/VU/S&F
FN. • More accurate than either test alone.
Complications
Mortality&
Morbidity
Specific risks
for PTB
neonate
• Shorter the term the
greater the risk.
• PT-premature ,is at risk
of death in 1st year of
life(infant)& mostly in 1st
month(neonatal)
• Neurological
• CVS
• Respiratory
• GIT &Metabolic
• Hematological
• Infection
Management
Progesterone & PTL
• Progesterone known as P4 (pregn-4-ene-3,20-dione) is
a C -21 steroid hormone involved in the female menstrual
cycle, pregnancy support and embryogenesis of humans.
• Progesterone consists of 4 interconnected cyclic
hydrocarbons .It contains ketone and oxygenated
functional groups ,as well as 2 methyl branches.
Medical applications
• Progesterone was approved by FDA as vaginal gel on July
1997, an oral capsule on May 1998 , injection form on April
2001 and as vaginal insert on June 2007.
• Other specific uses for progesterone
 L. Ph. Support in ART.
 Control persistent unovulatory Bl.
 Progesterone Withdrawal Bl.
 TTT multiple sclerosis.
 Has a role in skin elasticity & bone strength.
 Prevent conception or inducing abortion progest. receptor
antag. or SPRMs (RU486).
 Male behavior.
 a component of HRT for ttt of gender dysphoria.
Prevention of PTB; Vaginal progesterone
in women with a short cervix .
• Indeed PTL. & term labor share a common terminal
pathway , defined as anatomic, endocrinologic,
biochemical, and clinical events.
• An important diff. between term & PTL. is that the former
“physiologic activation of the common pathway, while the
later ( pathologic activation that extemporaneously activates
components of the common pathway).
Prevention of PTB; Vaginal progesterone
in women with a short cervix .
• The activation of UT. Components of the common pathway
may be synchronous or asynchronous.
 Synchronous clinical PTL
 Asynchronous diff. clinical presentation
(PPROM,Cx.insuff.,PT. Ut.contr.)
The preterm parturition syndrome
• The mechanisms of PTL shown in this figure, It is noted that
more than one mechanism may be operative in one patient.
Short Cervix
• A short cervix is syndromic in nature and can be caused by
multiple etiologies:
Technique for sonographic examination
of the uterine cervix
• Trans abdominal examination(not recommended )
due to:
o Requires distended bladder.
o A distended bladder compresses & artificially lengthen
Ut.cervix.
o A waiting room with patients having full bladder.
o The image quality.
o 45% of Patients with cx. Legnth ≤ 25mm would be missed.
Technique for sonographic examination
of the uterine cervix
• Tans abdominal examination(not recommended)
due to:
o Requires distended bladder.
o A distended bladder compresses & artificially lengthen
Ut.cervix.
o A waiting room with patients having full bladder.
o The image quality.
o 45% of Patients with cx. Legnth ≤ 25mm would be missed.
Technique for sonographic examination
of the uterine cervix
• Transabdominal sonogram performed in a patient with a full
bladder. The bladder is causing compression and artificial
lengthening of the uterine cervix (Adopted from: Romero et
al., 2013).
• Same patient but with the bladder emptied and transvaginal
sonography performed. Note that the true cervical length is
short (15.5 mm) (Adopted from: Romero et al., 2013).
Technique for sonographic examination
of the uterine cervix
• Transabdominal ultrasound when the fetus is in a vertex
presentation. Note that the image quality of the uterine
cervix is poor, which is due to the greater distance
between the probe and the cervix, and shadowing from
the fetal head (Adopted from: Romero et al., 2013).
Technique for sonographic examination
of the uterine cervix
• Transvaginal ultrasound of the uterine cervix (cervical
length 39.8 mm). This is the “gold standard” for the
performance of cervical examinations during pregnancy.
Note that the visualization of cervical anatomy and
measurement of the cervical length is optimal (Adopted
from: Romero et al., 2013).
parameter Group1 (IM) Group2 (Vaginal) Group 3 (Placebo) p
No. % No. % No. %
22-31 35 70 38 67 34 68
32-42 15 30 12 24 16 32
Mean+_ SD 29.3 28.9+_3.8 29.6+_3.7
0.6
Median (IQR) 29(25-34) 29(26-31) 30(27-32)
arameter Group1 Group2 Group3 P
No. % No. % NO. %
Working 29 58 26 52 32 64
0.6
House-wife 21 42 24 48 18 36
Parameter Group1 Group2 Group3 P
No. % No. % No. %
28-30 25 50 15 30 23 46
31-34 25 50 35 70 27 54
Mean+_ 30.8+_2.3 31.4+_2 30.9+_2.1
0.2
Median
(IQR)
28(29-33) 32(30-33) 31(29-33)
Parameter Group1 Group2 Group3 P
No. % No. % No. %
≤1500 10 20 8 16 10 20
≤2500 40 80 42 84 40 80
Mean+_SD 2385.3+_
596.4
2302.2+_
526.6
2238.6+_
573.4 0.3
Median
(IQR)
2627
(2540-2746)
2384
(1907-2640)
2500
(1869-2716)
Parameter Group1 Grouo2 Group3 P
No. % No. % No. %
Parous (with
prev.PTB)
18 36 16 32 19 38
Parous
(without PTB)
6 12 7 14 9 18
0.8
Nulliparous 26 52 27 54 22 44
Parameter Group1 Group2 Group3 p
No. % No. % No. %
White 41 82 43 86 45 90
Black 5 10 6 12 3 6
0.7
Others 4 8 1 2 2 2
Parameter Group1 Group2 Group3 P
No. % No. % No. %
18.5-25(n.) 17 34 24 48 19 38
25.1-30(O.W) 33 66 24 48 48 21
30.1-35(mod.Obese 2 4 7 14
35.1-40(severeObese) 3 6
0.2
Mean+_SD 26.1+_2.5 25.6+_2.4 27+_3.7
Median(IQR) 25.8(24.4-28.3) 25(24-27) 26(24-29)
Parameter Group1 Group2 Group3 P
No. % NO. % No. %
Single 45 90 43 86 42 84
0.5
Twin 5 10 7 14 8 16
Parameter Group1(IM Group2(vag) Group3( placebo p
Mean+_SD 20.8+_ 3.2 20.3+_3.5 20.7+_3
Median(IQR 21(18-23) 20(17-24) 21(18-23)
0.7
Comparison between the studied groups as regard 1ry & 2ry outcomes.
Parameter Group1(IM Group2(vag) Group3(placebo) p
No. % No. % No. %
1ry outcom 11 22 10 20 22 44 0.01
Fetal death 4 8 3 6 3 6 0.3
Neonatal death 1 2 0 0 1 2 1
IVH 4 8 5 10 3 6 0.8
RDS 7 14 8 16 4 8 0.5
ROP 3 6 3 6 3 6 o.6
NICU admission 13 26 14 28 11 22 0.6
Ventilation 6 12 5 10 3 6 0.7
Comparison between the studied groups as regards progesterone side
effects.
Parameter Group1(IM Group2(vag) P
Bloating 2 4 1 2 1
Fluid retention 2 4 1 2 1
Breast tenderness 8 16 10 20 0.3
Excessive Wt.gain 4 8 1 2 1
Nausea 6 12 2 4 1
Headache 6 12 4 8 1
Dizziness; Drowsiness 4 8 3 6 1
Difficulty of sleeping 2 4 2 4 1
Depression 2 4 1 2 1
Itching, Rash, Allergic
reaction
14 28 5 10
0.04
Vaginal irritation 0 0 20 40 0.001
DISCUSSION
 Prevention of PTB should be one of ANC, intervention for
preventing & ttt. PTB includes bed rest, cx. cerclage, and
progesterone and AB.
(FuKuyama et al.,2012)
 In the contemporary study , the rate of PTB among women
receiving vaginal progesterone from 20-24w until delivery
was 20% and 27.5% with IM progesterone .
 indicating that progesterone either vaginally or IM is highly
effective for prevention of PTB
Fonseca et al.,2003 Macknezie.,2006 Cetingoz et al., 2011
Berghella &Mackeen, 2011)
 Recent clinical studies depicted that progesterone is
effective even in the case of short cx. , it exerts effects by
inhibiting production of PG. & pro-inflammatory
cytokines (IL-8&IL-1B).
(Berghellaet al.,2010; Facchinetti et al.,2009)
 The current study demonstrated that there is no diff. in
the reduction of PTB in women (Vag.) & those (IM.)
 In this contemporaneous trial, the rate of S/E related to
Vag. Progesterone was lower compared with IM
progesterone .
Conclusions and Recommendations
• Our trial of progesterone administration
to pregnant women at risk of PTB with
short Cx.(15-20mm), predicted by TV
U/S seems to be effective, safe with
tolerable side effects.
• Route of Progesterone administration :
 Vaginal discharge, pruritus &
nausea
 IM bruises at injection site,
nausea, vomiting &hot flushes (Allergic
reactions).
Lastly, we concluded that
the effectiveness of
vaginal progesterone was
the same as IM with less
adverse effects.
preterm Labor and Progesterone

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preterm Labor and Progesterone

  • 1.
  • 2.
  • 3. L/O/G/O A thesis Submitted in Partial Fulfillment of the Requirements for (M.D.) in Obstetrics & Gynecology By Moataz Gamal Taha Abu-Shahba (2014) Specialist of Obstetrics &Gynecology Al-Galaa Teaching Hospital
  • 4. • Praise be to Allah, who exalted in knowledge whom he wills; but above those that have knowledge, there is one more knowing; to Him is the goal and to Him is the return of all. • Supervising Professors Especially Professor Fawzy Abel Aziz, Professor Mohamed Sherif El-Sayes and Dr. Mohamed Ibrahim Mostafa • My Family (Mother, brothers, wife, children). Acknowledgments
  • 6. Preterm labor  Birth of a baby of less than 37 weeks gestational age.  The cause is elusive and unknown.  The reduction of PTL is a challenging proposition.  PTB vs. premature birth.  PTB is among the top causes of death in infants worldwide.
  • 7. Epidemiology & Magnitude of The Problem  In Europe, PTB is generally 5-9% and in USA it has been risen to 12-13% in the last decades.(Goldenberg,2008).  It is estimated that one-third of LBW deliveries are due to preterm delivery.  PTB is a significant cost factor in healthcare including long term care for disabilities .  550.000 PTB each year in USA , run up 26$ billion , mostly related to NICU.
  • 9. Diagnosis Symptoms signs Initial Evaluation • Gestational age • ROM • Infection • In Labor • T/V U/S&/or FFN Assess ROM • Speculum ex. (sample for FFN, , alkalinity, nitrazine paper test Assess for infection • Urine sample(bacteriuria, &P.N.) • RectoVaginal culture(GBS) • Gonorrhea,B.V.,&T.V.
  • 10. Diagnosis True labor • Regular Uterine contra.+dilat. &effeac. +descent (3cm,80%,ROM& V.Bl.) FFN • -ve predictive value 99% • +ve predictive value 13-30% Aminosure® • One step immuno chromatographic assay.(PAMG-1) T/VU/S&F FN. • More accurate than either test alone.
  • 11. Complications Mortality& Morbidity Specific risks for PTB neonate • Shorter the term the greater the risk. • PT-premature ,is at risk of death in 1st year of life(infant)& mostly in 1st month(neonatal) • Neurological • CVS • Respiratory • GIT &Metabolic • Hematological • Infection
  • 13. Progesterone & PTL • Progesterone known as P4 (pregn-4-ene-3,20-dione) is a C -21 steroid hormone involved in the female menstrual cycle, pregnancy support and embryogenesis of humans. • Progesterone consists of 4 interconnected cyclic hydrocarbons .It contains ketone and oxygenated functional groups ,as well as 2 methyl branches.
  • 14. Medical applications • Progesterone was approved by FDA as vaginal gel on July 1997, an oral capsule on May 1998 , injection form on April 2001 and as vaginal insert on June 2007. • Other specific uses for progesterone  L. Ph. Support in ART.  Control persistent unovulatory Bl.  Progesterone Withdrawal Bl.  TTT multiple sclerosis.  Has a role in skin elasticity & bone strength.  Prevent conception or inducing abortion progest. receptor antag. or SPRMs (RU486).  Male behavior.  a component of HRT for ttt of gender dysphoria.
  • 15. Prevention of PTB; Vaginal progesterone in women with a short cervix . • Indeed PTL. & term labor share a common terminal pathway , defined as anatomic, endocrinologic, biochemical, and clinical events. • An important diff. between term & PTL. is that the former “physiologic activation of the common pathway, while the later ( pathologic activation that extemporaneously activates components of the common pathway).
  • 16. Prevention of PTB; Vaginal progesterone in women with a short cervix . • The activation of UT. Components of the common pathway may be synchronous or asynchronous.  Synchronous clinical PTL  Asynchronous diff. clinical presentation (PPROM,Cx.insuff.,PT. Ut.contr.)
  • 17. The preterm parturition syndrome • The mechanisms of PTL shown in this figure, It is noted that more than one mechanism may be operative in one patient.
  • 18. Short Cervix • A short cervix is syndromic in nature and can be caused by multiple etiologies:
  • 19. Technique for sonographic examination of the uterine cervix • Trans abdominal examination(not recommended ) due to: o Requires distended bladder. o A distended bladder compresses & artificially lengthen Ut.cervix. o A waiting room with patients having full bladder. o The image quality. o 45% of Patients with cx. Legnth ≤ 25mm would be missed.
  • 20. Technique for sonographic examination of the uterine cervix • Tans abdominal examination(not recommended) due to: o Requires distended bladder. o A distended bladder compresses & artificially lengthen Ut.cervix. o A waiting room with patients having full bladder. o The image quality. o 45% of Patients with cx. Legnth ≤ 25mm would be missed.
  • 21. Technique for sonographic examination of the uterine cervix • Transabdominal sonogram performed in a patient with a full bladder. The bladder is causing compression and artificial lengthening of the uterine cervix (Adopted from: Romero et al., 2013). • Same patient but with the bladder emptied and transvaginal sonography performed. Note that the true cervical length is short (15.5 mm) (Adopted from: Romero et al., 2013).
  • 22. Technique for sonographic examination of the uterine cervix • Transabdominal ultrasound when the fetus is in a vertex presentation. Note that the image quality of the uterine cervix is poor, which is due to the greater distance between the probe and the cervix, and shadowing from the fetal head (Adopted from: Romero et al., 2013).
  • 23. Technique for sonographic examination of the uterine cervix • Transvaginal ultrasound of the uterine cervix (cervical length 39.8 mm). This is the “gold standard” for the performance of cervical examinations during pregnancy. Note that the visualization of cervical anatomy and measurement of the cervical length is optimal (Adopted from: Romero et al., 2013).
  • 24.
  • 25.
  • 26.
  • 27.
  • 28.
  • 29.
  • 30. parameter Group1 (IM) Group2 (Vaginal) Group 3 (Placebo) p No. % No. % No. % 22-31 35 70 38 67 34 68 32-42 15 30 12 24 16 32 Mean+_ SD 29.3 28.9+_3.8 29.6+_3.7 0.6 Median (IQR) 29(25-34) 29(26-31) 30(27-32)
  • 31. arameter Group1 Group2 Group3 P No. % No. % NO. % Working 29 58 26 52 32 64 0.6 House-wife 21 42 24 48 18 36
  • 32. Parameter Group1 Group2 Group3 P No. % No. % No. % 28-30 25 50 15 30 23 46 31-34 25 50 35 70 27 54 Mean+_ 30.8+_2.3 31.4+_2 30.9+_2.1 0.2 Median (IQR) 28(29-33) 32(30-33) 31(29-33)
  • 33. Parameter Group1 Group2 Group3 P No. % No. % No. % ≤1500 10 20 8 16 10 20 ≤2500 40 80 42 84 40 80 Mean+_SD 2385.3+_ 596.4 2302.2+_ 526.6 2238.6+_ 573.4 0.3 Median (IQR) 2627 (2540-2746) 2384 (1907-2640) 2500 (1869-2716)
  • 34. Parameter Group1 Grouo2 Group3 P No. % No. % No. % Parous (with prev.PTB) 18 36 16 32 19 38 Parous (without PTB) 6 12 7 14 9 18 0.8 Nulliparous 26 52 27 54 22 44
  • 35. Parameter Group1 Group2 Group3 p No. % No. % No. % White 41 82 43 86 45 90 Black 5 10 6 12 3 6 0.7 Others 4 8 1 2 2 2
  • 36. Parameter Group1 Group2 Group3 P No. % No. % No. % 18.5-25(n.) 17 34 24 48 19 38 25.1-30(O.W) 33 66 24 48 48 21 30.1-35(mod.Obese 2 4 7 14 35.1-40(severeObese) 3 6 0.2 Mean+_SD 26.1+_2.5 25.6+_2.4 27+_3.7 Median(IQR) 25.8(24.4-28.3) 25(24-27) 26(24-29)
  • 37. Parameter Group1 Group2 Group3 P No. % NO. % No. % Single 45 90 43 86 42 84 0.5 Twin 5 10 7 14 8 16
  • 38. Parameter Group1(IM Group2(vag) Group3( placebo p Mean+_SD 20.8+_ 3.2 20.3+_3.5 20.7+_3 Median(IQR 21(18-23) 20(17-24) 21(18-23) 0.7
  • 39. Comparison between the studied groups as regard 1ry & 2ry outcomes. Parameter Group1(IM Group2(vag) Group3(placebo) p No. % No. % No. % 1ry outcom 11 22 10 20 22 44 0.01 Fetal death 4 8 3 6 3 6 0.3 Neonatal death 1 2 0 0 1 2 1 IVH 4 8 5 10 3 6 0.8 RDS 7 14 8 16 4 8 0.5 ROP 3 6 3 6 3 6 o.6 NICU admission 13 26 14 28 11 22 0.6 Ventilation 6 12 5 10 3 6 0.7
  • 40.
  • 41. Comparison between the studied groups as regards progesterone side effects. Parameter Group1(IM Group2(vag) P Bloating 2 4 1 2 1 Fluid retention 2 4 1 2 1 Breast tenderness 8 16 10 20 0.3 Excessive Wt.gain 4 8 1 2 1 Nausea 6 12 2 4 1 Headache 6 12 4 8 1 Dizziness; Drowsiness 4 8 3 6 1 Difficulty of sleeping 2 4 2 4 1 Depression 2 4 1 2 1 Itching, Rash, Allergic reaction 14 28 5 10 0.04 Vaginal irritation 0 0 20 40 0.001
  • 42.
  • 44.  Prevention of PTB should be one of ANC, intervention for preventing & ttt. PTB includes bed rest, cx. cerclage, and progesterone and AB. (FuKuyama et al.,2012)  In the contemporary study , the rate of PTB among women receiving vaginal progesterone from 20-24w until delivery was 20% and 27.5% with IM progesterone .  indicating that progesterone either vaginally or IM is highly effective for prevention of PTB Fonseca et al.,2003 Macknezie.,2006 Cetingoz et al., 2011 Berghella &Mackeen, 2011)
  • 45.  Recent clinical studies depicted that progesterone is effective even in the case of short cx. , it exerts effects by inhibiting production of PG. & pro-inflammatory cytokines (IL-8&IL-1B). (Berghellaet al.,2010; Facchinetti et al.,2009)  The current study demonstrated that there is no diff. in the reduction of PTB in women (Vag.) & those (IM.)  In this contemporaneous trial, the rate of S/E related to Vag. Progesterone was lower compared with IM progesterone .
  • 47. • Our trial of progesterone administration to pregnant women at risk of PTB with short Cx.(15-20mm), predicted by TV U/S seems to be effective, safe with tolerable side effects. • Route of Progesterone administration :  Vaginal discharge, pruritus & nausea  IM bruises at injection site, nausea, vomiting &hot flushes (Allergic reactions).
  • 48. Lastly, we concluded that the effectiveness of vaginal progesterone was the same as IM with less adverse effects.