I don’t seem to understand these hcg levels. I did a blood test the first time and it showed that my hcg levels were on 6105 and I am 5 weeks pregnant. I did a test again a week after and it shows 1501 hcg levels and my nurse says I am 6 weeks 2 days pregnant. Exactly what could it be because isn’t the number supposed to be higher at 6 weeks
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Dear Patients,
I created this forum to welcome any questions you have on the topic of infertility, IVF, conception, testing, evaluation, or any related topics. I do my best to answer all questions in less than 24 hours. I know your question is important and, in many cases, I will answer within just a few hours. Thank you for taking the time to trust me with your concern.– Geoffrey Sher, MD
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Hcg levels
Name: Nomonde M
I don’t seem to understand these hcg levels. I did a blood test the first time and it showed that my hcg levels were on 6105 and I am 5 weeks pregnant. I did a test again a week after and it shows 1501 hcg levels and my nurse says I am 6 weeks 2 days pregnant. Exactly what could it be because isn’t the number supposed to be higher at 6 weeks
Answer:
Ideally the level should have increased. Repeat the hCG again.
Geoff Sher
TIMING AND INTERPRETATION OF hCG BLOOD PREGNANCY TESTS
Geoffrey Sher MD
Going through IVF is a major investment, emotionally, physically, and financially, for every patient or couple. One of the most crucial moments is receiving the result of the blood test for human chorionic gonadotropin (hCG) pregnancy. It’s a big deal! The days after the embryo transfer, waiting for this result, can be extremely stressful. That’s why it’s crucial for the IVF doctor and staff to handle this information with care and professionalism. They should be accessible to the patient/couple and provide results promptly and sensitively.
Testing urine or blood to check for human chorionic gonadotropin (hCG) is the best way to confirm pregnancy. Urine tests are cheaper and more commonly used. They are also more convenient because they can be done anywhere. However, blood tests are more reliable and sensitive than urine tests. They can detect pregnancy earlier and at lower hCG levels. Blood tests are also more accurate and can track changes in hCG levels over time. Urine tests can detect hCG when blood levels are above 20IU, which is about 16-18 days after ovulation or 2-3 days after a missed period. Blood tests can measure any concentration of hCG about 12-13 days after ovulation.
Detecting hCG in the blood early on and tracking its increase is especially useful for women undergoing fertility treatments like controlled ovarian stimulation or in vitro fertilization. The sooner hCG is detected and measured, the more information can be gathered about the success of implantation and the health of the developing embryo.
Typically, two beta hCG blood tests are done, spaced 2-4 days apart. It’s best to wait for the results of the second test before reporting on the pregnancy. This is because an initial result can change, even from equivocal or negative to positive. Sometimes a normal embryo takes longer to implant, and the hCG level can be initially low or undetectable. Regardless of the initial level, the test should be repeated after two days to check for a significant rise in hCG. A significant rise usually indicates that an embryo is implanting, which suggests a possible pregnancy. Waiting for the second test result helps avoid conveying false hope or disappointment.
It’s important to note that beta hCG levels don’t double every two days throughout pregnancy. Once the levels rise above 4,000U, they tend to increase more slowly. Except in specific cases like IVF using an egg donor or transfer of genetically tested embryos, the birth rate following IVF in younger women is around 40% per embryo transfer. Patients need to have realistic expectations and should be informed about how and when they will receive the news, as well as counseling in case of a negative outcome.
When an embryo starts to implant, it releases the pregnancy hormone hCG into the woman’s bloodstream. Around 12 days after egg retrieval, 9 days after a day 3 embryo transfer, or 7 days after a blastocyst transfer, a woman should have a quantitative beta hCG blood pregnancy test performed. By that time, most of the hCG injected to prepare the eggs for retrieval should have cleared from the bloodstream. So, if the test detects more than 10 IU of hCG per ml of blood, it indicates that the embryo has attempted to implant. In third-party IVF (e.g., ovum donation, gestational surrogacy, embryo adoption, or frozen embryo transfers), no hCG trigger is administered, so any amount of hCG detected in the blood is considered significant.
Sometimes, there is a slow initial rise in hCG between the first and second tests (failure to double every 48 hours). In such cases, a third and sometimes a fourth hCG test should be done at two-day intervals. A failure to double on the third and/or fourth test is a poor sign and could indicate a failed or dysfunctional implantation. In some cases, a progressively slow rising hCG level might indicate an ectopic pregnancy, which requires additional testing and follow-up.
In certain situations, the first beta hCG level starts high, drops with the second test, and then starts doubling again. This could suggest that initially, multiple embryos started to implant but only one survived to continue a healthy implantation.
It’s customary for the IVF clinic staff to inform the patient/couple and the referring physician about the hCG pregnancy test results. Often, the IVF physician or nurse-coordinator coordinates with the referring physician to arrange all necessary pregnancy tests. If the patient/couple prefer to make their own arrangements, the program should provide detailed instructions.
In some cases, when the two blood pregnancy tests show that one or more embryos are implanting, certain programs recommend daily injections of progesterone or the use of vaginal hormone suppositories for several weeks to support the implantation process. Others give hCG injections three times a week until the pregnancy can be confirmed by ultrasound examination. Some IVF programs don’t prescribe any hormones after the embryo transfer.
Patients with appropriate doubling of hCG levels within two days after frozen embryo transfer (FET) or third-party IVF procedures such as surrogacy or egg donation may receive estradiol and progesterone injections, often along with vaginal hormone suppositories, for 10 weeks after the implantation is diagnosed by blood pregnancy testing.
A positive Beta hCG blood pregnancy test indicates the possibility of conception, but ultrasound confirmation is needed to confirm the pregnancy. Until then, it is referred to as a “chemical pregnancy.” Only when ultrasound examination confirms the presence of a gestational sac, clinical examination establishes a viable pregnancy, or after abortion when products of conception are detected, is it called a clinical intrauterine pregnancy.
A significantly elevated hCG blood level without concomitant detection of an gestational sac inside the uterus by ultrasound after 5 weeks gestation raises the suspicion of an ectopic (tubal) pregnancy.
The risk of miscarriage gradually decreases once a viable clinical pregnancy is diagnosed (a conceptus with a regular heartbeat of 110-180 beats per minute). From this point onward, the risk of miscarriage is usually 10- 15% for women under 40 years old and around 35% for women in their early forties.
Dealing with successful IVF cases is relatively easy as everyone feels happy and validated. The real challenge lies in handling unsuccessful cases. Setting rational expectations from the beginning is crucial. In some cases (fortunately rare), emotional pressure may overwhelm the patient/couple, leading to a need for counseling or psychiatric therapy. I always advise my patients that receiving optimal care doesn’t always guarantee the desired outcome. There are many variables beyond our control, especially the unpredictable nature of fate. With around 36 years of experience in this field, I strongly believe that when it comes to IVF, the saying “man proposes while God disposes” always holds.
There are a few important things to consider when interpreting blood hCG levels. Levels can vary widely, ranging from 5mIU/ml to over 400mIU/ml, 10 days after ovulation or egg retrieval. The levels double every 48-72 hours until the 6th week of pregnancy, after which the doubling rate slows down to about 96 hours. By the end of the 1st trimester, hCG levels reach 13,000-290,000 IU and then slowly decline to around 26,000-300,000 IU at full term. Here are the average hCG levels during the first trimester:
- 3 weeks after the last menstrual period (LMP): 5-50 IU
- 4 weeks LMP: 5-426 IU
- 5 weeks LMP: 18-7,340 IU
- 6 weeks LMP: 1,080-56,500 IU
- 7-8 weeks LMP: 7,650-229,000 IU
- 9-12 weeks LMP: 25,700-288,000 IU
Most doctors wait until around the 7th week to perform an ultrasound to confirm pregnancy. By that time, the heartbeat should be clearly visible, providing a more reliable assessment of the pregnancy’s viability.
In some cases, blood hCG levels can be unusually high or increase faster than normal. This could indicate multiple pregnancies or a molar pregnancy. Rarely, conditions unrelated to pregnancy, such as certain ovarian tumors or cancers, can cause detectable hCG levels in both blood and urine.
To summarize, testing urine or blood for hCG is the most reliable way to confirm pregnancy. Urine tests are more common and convenient, while blood tests are more accurate and can detect pregnancy earlier. Tracking hCG levels in the blood is especially important for women undergoing fertility treatments. It’s essential to wait for the results of a second blood test before confirming pregnancy to avoid false hope or disappointment. Interpreting hCG levels requires considering various factors, and doctors usually perform an ultrasound around the 7th week for a more accurate assessment. Unusually high hCG levels may indicate multiple pregnancies or other conditions unrelated to pregnancy. Providing sensitive and timely communication of results is crucial for IVF clinics to support patients through the emotional journey.
______________________________________________________
Herewith are online links to 2 E-books recently co-authored with my partner at SFS-NY (Drew Tortoriello MD)……. for your reading pleasure:
- From In Vitro Fertilization to Family: A Journey with Sher Fertility Solutions (SFS) ; https://sherfertilitysolutions.com/sher-fertility-solutions-ebook.pdf
- Recurrent Pregnancy Loss and Unexplained IVF Failure: The Immunologic Link ;https://drive.google.com/file/d/1iYKz-EkAjMqwMa1ZcufIloRdxnAfDH8L/view
I invite you to visit my very recently launched “Podcast”, “HAVE A BABY” on RUMBLE; https://rumble.com/c/c-3304480
If you are interested in having an online consultation with me, please contact my assistant, Patti Converse at 702-533-2691 or email her at concierge@sherivf.com\
Reconstrucción de trompas
Name: Nora R
Hace 7 años me hice una ligadura de trompas con mi última hija en mi país. Tengo 2 niñas. Ahora deseo tener un bebé. Tengo 30 años. Quiero saber el precio de la reconstrucción de trompas.
Author
Answer:
Please post your question in English!
Geoff Sher
_________________________________________________________________________________
PLEASE SHARE THIS WITH OTHERS AND HELP SPREAD THE WORD!!
Herewith are online links to 2 E-books recently co-authored with my partner at SFS-NY (Drew Tortoriello MD)……. for your reading pleasure:
- From In Vitro Fertilization to Family: A Journey with Sher Fertility Solutions (SFS) ; https://sherfertilitysolutions.com/sher-fertility-solutions-ebook.pdf
- Recurrent Pregnancy Loss and Unexplained IVF Failure: The Immunologic Link ;https://drive.google.com/file/d/1iYKz-EkAjMqwMa1ZcufIloRdxnAfDH8L/view
I invite you to visit my very recently launched “Podcast”, “HAVE A BABY” on RUMBLE; https://rumble.com/c/c-3304480
If you are interested in having an online consultation with me, please contact my assistant, Patti Converse at 702-533-2691 or email her at concierge@sherivf.com\
Elevated dhea
Name: Julie A
I just Received blood work where my dhea levels are elevated and they might believe it’s associate with pcos. What can I do In regards to having a baby?
Author
Answer:
Raised DHEA is not a real problem . it is a raised DHEAS that xcouyld be problematic as it would point to a possible adrenal contribution to the PCOS equation.
Navigating Polycystic Ovary Syndrome: Understanding, Hope, and Treatment
Geoffrey Sher MD
Understanding the intricate interplay of hormones and the impact on egg development empowers us to create personalized protocols, offering hope for improved egg quality and ultimately optimizing the chances of successful IVF for women with PCOS.
Polycystic ovary syndrome (PCOS) is a widespread hormonal disorder affecting 5% to 10% of reproductive-age women globally. Women with PCOS often have enlarged ovaries containing multiple small fluid-filled collections (micro-cysts) arranged in a “string of pearls” pattern below the ovarian surface, intertwined with an overgrowth of ovarian connective tissue.
PCOS is marked by abnormal ovarian function causing absent, irregular or dysfunctional ovulation and menstruation, infertility, increased body hair (hirsutism), acne, and higher body weight as indicated by an above normal body mass index (BMI).
Despite substantial research efforts to identify its cause, the origins of PCOS remain elusive, and a definite cure is yet to be found. This disorder is notably diverse and often has a genetic basis within families.
Infertility related to PCOS is attributed to various factors, including irregular gonadotropin (FSH and LH) pituitary secretion, peripheral insulin resistance, elevated levels of adrenal and/or ovarian androgens (male hormones), and dysfunction in growth factors. Individuals with PCOS often battle obesity and insulin resistance. The compensatory surge in insulin levels further stimulates ovarian androgen production, potentially hampering egg maturation. Notably, the degree of insulin resistance is closely linked to anovulation.
PCOS also poses long-term health risks, underscoring the need for vigilant annual health check-ups to monitor potential conditions like non-insulin-dependent diabetes mellitus, hypertension, hypercholesterolemia, cardiovascular disease, and endometrial cancer.
Though PCOS-related infertility is typically manageable with fertility drugs, lifestyle modifications involving diet and exercise are fundamental for long-term management. Recent advancements have shown improvements in ovulation rates, androgen levels, pregnancy rates, and even a reduction in first-trimester miscarriage rates through the use of insulin sensitizers like Metformin to address underlying insulin resistance.
Most PCOS patients are young and often experience successful pregnancies with oral clomiphene or Letrozole/Femara. However, a subset of PCOS patients with severe ovarian ovulatory dysfunction and those requiring IVF treatment, will usually require injectable gonadotropin medications such as Follistim, Gonal-F, Menopur, etc. These treatments can trigger an exaggerated response to gonadotropins, potentially leading to complications such as Severe Ovarian Hyperstimulation Syndrome (OHSS) and high-order multiple births ( triplets or greater). For these cases, employing strategies like “prolonged coasting” (see below) and/or delaying embryo transfer for a month or two in order to allow the ovaries to recover from ovarian stimulation, and selectively transferring fewer embryos present clear advantages..
PCOS and Egg/Embryo Quality:
PCOS and Egg/Embryo “Competency”.
A woman’s potential for successful egg maturation and embryo development is largely determined by genetics. However, this potential can also be significantly influenced by hormonal changes within the ovaries during the pre-ovulatory phase of her menstrual cycle. Achieving the right stimulation of the follicles and precise timing for egg maturation with the LH (Luteinizing Hormone) “surge” or through hCG (human chorionic gonadotropin) administration is crucial for optimal egg quality, fertilization, and subsequent embryo development.
Two key hormones, LH and FSH (follicle stimulating hormone), play vital but distinct roles in the development of eggs and follicles. FSH mainly stimulates granulosa cells (lining the follicles) and estrogen production (E2). On the other hand, LH primarily acts on the ovarian stroma (connective tissue around the follicle) to produce androgens ( predominantly testosterone and androstenedione). While a small amount of androgen supports egg and follicle development, excessive exposure can be harmful. Too much androgen can also hinder estrogen-induced growth of the uterine lining.
PCOS is commonly associated with elevated LH levels, leading to excess stromal growth, follicle overgrowth (referred to as cysts), and heightened androgen production. Accordingly, suppressing LH secretion using gonadotropin releasing hormone (GnRH) agonists like Lupron/ Buserelin/Superfact and decapeptyl proves beneficial. However, it is important to understand that some LH is essential for optimal egg and follicle development. Excessive LH on the other hand results in over-production of LH-induced ovarian androgens, which upon reaching the follicular fluid often compromises both follicle and egg development. Consequently, PCOS women who commonly over-produce LH and ovarian androgens frequently propagate poorly developed follicles and “dysmature/immature” eggs leading to poor fertilization and embryo quality as well as an androgen-induced insufficient uterine lining that might prejudice embryo implantation, It is in my opinion, that the compromised egg quality is not necessarily due to an inherent “egg defect “ but rather due to an adverse ovarian hormonal milieu which can often be avoided by tailoring stimulation protocols so as to avoid excessive LH-induced androgens, Avoiding .
Varieties of PCOS:
Polycystic Ovary Syndrome (PCOS) comes in various forms, each requiring tailored treatment. Here, I wish to shed light on the main types and how infertility linked to ovulation dysfunction can be managed.
- Hypothalamic-Pituitary-PCOS:
- Most common form with genetic roots.
- Characterized by high levels of Luteinizing Hormone (LH) and androgen hormones.
- Often associated with insulin resistance.
- Adrenal PCOS:
- Excess male hormones come from overactive adrenal glands.
- Elevated testosterone and/or androstenedione levels, along with increased dehydroepiandrosterone (DHEAS) levels, confirm diagnosis.
- Pelvic Adhesive Disease-Related PCOS:
- Linked to severe endometriosis, pelvic inflammatory disease, or extensive pelvic surgery.
- Lower response to ovulation induction.
- Notably, DHEAS levels remain unaffected.
Treating Infertility Due to Ovulation Dysfunction:
- Hypothalamic-Pituitary-/Ovarian PCOS:
- Successful treatment with fertility drugs like clomiphene citrate, Letrozole, or gonadotropins.
- In-vitro Fertilization (IVF) is increasingly favored.
- Oral Metformin can help reduce insulin resistance and androgen levels.
- Adrenal PCOS:
- Treated with steroids like prednisone or dexamethasone to suppress adrenal androgen production.
- Combined with fertility drugs for induced ovulation.
- PCOS due to Pelvic Adhesive Disease:
- Often linked to compromised ovarian reserve and higher FSH levels.
- Requires high doses of gonadotropins and “estrogen priming” for effective ovulation induction or IVF.
The Risks of Treatment
- High-order multiple pregnancies (triplets, or greater):
PCOS patients undergoing ovulation induction are at greater risk of multiple pregnancies which are especially treacherous both mother and offspring occur with the occurrence of high-order multiple pregnancies. This risk is not preventable when ovulation induction alone is used (with or without IUI) since there is no ability to regulate the number of eggs that are ovulated. Conversely, IVF allows for the number of embryos transferred to the uterus to be deliberately regulated.
- Severe Ovarian Hyperstimulation (OHSS)
- OHSS is a significant concern for women with PCOS undergoing fertility treatments , especially where gonadotropins are administered for ovarian stimulation.
- Understanding OHSS:
- Women with PCOS tend to hyper-respond to fertility drugs, often producing excessive ovarian follicles.;
- his can escalate into OHSS, posing life-threatening risks.
Indicators of OHSS:
- OHSS begins with an abundance of ovarian follicles (often more than 25).
- Rapid rise in estradiol (E2) levels, sometimes exceeding 3000pg/ml within 7-9 days of stimulation.
- The risk of OHSS exceeds 80% when the peak blood estradiol level exceeds 6000pg/ml.
Symptoms and Signs of OHSS:
- Abdominal swelling due to fluid accumulation (ascites).
- Sometimes fluid in the chest cavity (hydrothorax) and even around the heart ( pericardial effusion)
- Rapid weight gain (more than a pound per day) due to fluid retention.
- Abdominal pain and lower backache.
- Nausea, diarrhea, and vomiting.
- Visual disturbances like blurred vision and spots in front of the eyes.
- Reduced urine output.
- Cardiovascular complications and bleeding tendencies.
Managing OHSS:
- If fluid accumulation compromises breathing, elevating the head of the bed often helps.
- Drainage of excess fluid through transvaginal sterile needle aspiration (vaginal paracentesis) may be necessary.
- Symptoms typically subside within 10-12 days of hCG shot if pregnancy doesn’t occur or by the 8th week of pregnancy.
- Monitor urine output and perform chest X-rays and blood tests regularly to assess the condition.
- In severe cases, hospitalization and intensive care might be necessary.
Avoiding OHSS while protecting egg quality though “Prolonged Coasting”
In the early 1990s, I introduced a game-changing approach to the prevention of OHSS, called “Prolonged Coasting” (PC) . The method avoids the life-endangering risks associated with this complication while to largely protecting egg quality . PC has now become a standard treatment for OHSS prevention. However, the effective success of PC is very largely dependent on meticulous implementation and proper timing.
What is “Prolonged Coasting” (PC)?
- PC involves a strategic pause in administering gonadotropin therapy, while continuing GnRHa (Lupron/Buserelin/Superfact/decapeptyl)
- This method significantly reduces the risk of OHSS, a life-threatening condition associated with excessive follicle growth.
- Balancing Act for Egg Quality:
- While PC is highly effective in averting OHSS, concerns were raised about potential impacts on fertilization rates and embryo implantation.
- Experience suggests that the perceived egg/embryo quality deficit isn’t directly caused by PC but is more about precise timing.
- Timing is Crucial: It is initiated when a woman with >25 follicles (total) with an estradiol measurement of >2500pg/ml has at least 50% of her follicles at 14mm diameter. It ends when the rising E2 plateaus and then drops. The key is to wait until the plasma estradiol concentration drops below 2,500 pg/ml before administering hCG. Initiating PC too early or too late can either halt follicle growth abruptly or lead to cystic follicles, both affecting egg quality. The timing allows for a progressive rise in estradiol levels followed by a plateau before a controlled decline, optimizing egg maturation. Even if the estradiol level falls below 1,000 pg/ml by hCG trigger time, resisting the urge to trigger prematurely with hCG is vital. This ensures eggs have adequate time for optimal development, increasing the chances of successful fertilization and embryo quality.
:
Words of caution:
- Pituitary suppression with GnRH antagonists (Ganirelix, Cetrotide, Orgalutron) can falsely suppress E2 levels and in my opinion, is not be suitable, especially in cases like PCOS a decision on timing for PC in large part hinges on the accurate determination of serial blood estradiol levels…Accordingly, I caution against their use in patients with PCOS where “prolonged coasting is contemplated being used.
- The standard practice of administering hCG (human chorionic gonadotropin) in an attempt to prematurely arrest further follicle growth and so prevent Severe Ovarian Hyperstimulation Syndrome (OHSS) can, by abruptly halting egg development, impact their maturation, prejudice their “competency” and in turn compromise embryo competency”, as well. Mastering the art of “Prolonged Coasting” is a critical step forward in fertility treatments. Precise timing and a patient-centered approach can make a world of difference, providing hope and improved outcomes for women on their journey towards motherhood.
In summary, when it comes to managing infertility in PCOS women, it is crucial to tailor stimulation protocols during IVF to minimize exposure to excessive LH-induced ovarian androgens. By limiting the use clomiphene snd Letrozole/Femara as well as LH-containing gonadotropins like Menopur and incorporating “prolonged coasting,” we can provide the necessary time for optimal follicle and egg development before administering hCG. This approach can potentially enhance egg quality and improve outcomes in IVF for women with PCOS.
_____________________________________________________________________
Herewith are online links to 2 E-books recently co-authored with my partner at SFS-NY (Drew Tortoriello MD)……. for your reading pleasure:
- From In Vitro Fertilization to Family: A Journey with Sher Fertility Solutions (SFS) ; https://sherfertilitysolutions.com/sher-fertility-solutions-ebook.pdf
- Recurrent Pregnancy Loss and Unexplained IVF Failure: The Immunologic Link ;https://drive.google.com/file/d/1iYKz-EkAjMqwMa1ZcufIloRdxnAfDH8L/view
I invite you to visit my very recently launched “Podcast”, “HAVE A BABY” on RUMBLE; https://rumble.com/c/c-3304480
If you are interested in having an online consultation with me, please contact my assistant, Patti Converse at 702-533-2691 or email her at concierge@sherivf.com\
embryo adoption
Name: shontae s
nd can use own eggs/embryos.
I am a current patient. 2 failed ivf. High NK. Myself and husband have 2 variants of MTHFR I did intralipids in both. I was wondering if we would have better chances if we used a donor embryo vs using embryo we have using my husbands sperm. With that said do you recommend a donor embryo site or do you have donor embryos that are best suited for us?
Author
Answer:
No, I do not think you need to go on Lovenox and use own eggs/embryos.
Hereditary Clotting Defects (Thrombophilia)
Geoffrey Sher MD
Thrombophilia (Hereditary Clotting Defect) is defined as the genetic predisposition to developing intravascular thrombosis. It is due to hypercoagulability of blood leading to impairment of initial vascularization that takes place during implantation.
Thrombophilia affects as many as one in five people in the United States and is responsible for pregnancy loss (most particularly after the 1st trimester) and “unexplained” infertility, as well as being a factor in some cases of “unexplained” IVF failure. Whether (and/or the extent to which) thrombophilia causes 1st trimester recurrent pregnancy loss (RPL) is the subject of debate and is controversial. In fact, first-trimester RPL is far more likely to be due to immunologic implantation dysfunction (IID) and/or irregularities in the contour of the uterine cavity or insufficient thickness of its lining (a thin endometrium). Thrombophilia has also been associated with late pregnancy-induced complications such as preeclampsia, premature separation of the placenta (abruptio placenta), placental insufficiency with intrauterine growth retardation, and in “unexplained” intrauterine death.
This having been said, it is a fact that most women with a thrombophilia go on to experience healthy pregnancies.
Diagnosis of Throbophilia
Thrombophilia is diagnosed when one or more of the following is detected:
- Mutational defect involving methylenetetrahydrofolate reductase (MTHFR), which occurs in at least 20% of affected cases. Homozygosity for a common C677T mutation in the MTHFR gene that is associated with hyperhomocysteinemia is the most common form of hereditary thrombophilia leading to a 3-fold increase in risk of complications.
- Mutation of factor V Leiden (FVL),
- A mutation of prothrombin G20210A,
- Deficiency of antithrombin III
- Deficiency of protein C
- Deficiency of protein S
Risk Factors
- Pregnant women with predisposing factors such as:
- A personal or family history of thromboembolism (deep vein thrombosis), pulmonary embolism (blood clot in the lung), cerebrovascular accidents (i.e. strokes)
- A personal history of pregnancy complications such as unexplained intrauterine death, preeclampsia, abruptio placenta, intrauterine growth retardation, placental insufficiency, should be tested for the condition.
Treatment
Treatment should be initiated as soon as possible after pregnancy is diagnosed biochemically (blood or urine hCG test) and be continued throughout gestation.
Severe thrombophilias (e.g. homozygous MTHFR mutations, protein C deficiency, prothrombin G20210A mutation) as well as cases of mild thrombophilias associated with one or more of the pregnancy complications mentioned above, are best treated with low-molecular weight heparin (LMWH) taken throughout pregnancy.
For other (milder) thrombophilias and no history of prior pregnancy complications: Low-dose aspirin with the B vitamins folic acid, B6 and B12.
_________________________________________________________________________________________________________________
Herewith are online links to 2 E-books recently co-authored with my partner at SFS-NY (Drew Tortoriello MD)……. for your reading pleasure:
- From In Vitro Fertilization to Family: A Journey with Sher Fertility Solutions (SFS) ; https://sherfertilitysolutions.com/sher-fertility-solutions-ebook.pdf
- Recurrent Pregnancy Loss and Unexplained IVF Failure: The Immunologic Link ;https://drive.google.com/file/d/1iYKz-EkAjMqwMa1ZcufIloRdxnAfDH8L/view
I invite you to visit my very recently launched “Podcast”, “HAVE A BABY” on RUMBLE; https://rumble.com/c/c-3304480
Doppler US – notch right at 13 weeks
Name: Cassidy O
Hello Dr Sher,
I hope you’re well.
We just had a dating scan at 13w1d, they confirmed everything looks good. However, in the printed report, it states that for the Dopler Ultrasound there is a “notch right” – they didn’t discuss this with us, but the PI left reading was 0.780 and the PI Right reading was 1.255, mean PI was 1.255, suggesting there is an imbalance.. does the mean potential hypertension/preeclampsia later on in pregnancy? Is there anything I could do to improve the position, to the extent it needs to be improved.. I’m taking 75mg of baby aspirin perhaps 150mg would be help.
I look forward to your reply.
Many thanks and best regards,
Gemma
Author
Answer:
Frankly, I would not be overly concerned. And no,there is in my opinion nothing to do here. except follow up with ultrasound evaluations intermittently.
Good luck!
Geoff Sher
___________________________________________________________
Herewith are online links to 2 E-books recently co-authored with my partner at SFS-NY (Drew Tortoriello MD)……. for your reading pleasure:
- From In Vitro Fertilization to Family: A Journey with Sher Fertility Solutions (SFS) ; https://sherfertilitysolutions.com/sher-fertility-solutions-ebook.pdf
- Recurrent Pregnancy Loss and Unexplained IVF Failure: The Immunologic Link ;https://drive.google.com/file/d/1iYKz-EkAjMqwMa1ZcufIloRdxnAfDH8L/view
I invite you to visit my very recently launched “Podcast”, “HAVE A BABY” on RUMBLE; https://rumble.com/c/c-3304480
If you are interested in having an online consultation with me, please contact my assistant, Patti Converse at 702-533-2691 or email her at concierge@sherivf.com\
Egg freezing risks in IVF
Name: Lisa-Marie E
Hello Dr. Sher
I am 39, childless and I’m currently undergoing IVF in Portugal. I have had 4 miscarriages in the past (2 clinical and 2 chemicals). On my last scan, my AFC was 15. My AMH is 1.24.
I would like to make and store as many embryos as possible in back-to-back retrievals, as we will be doing PGTA testing on the embryos and I know many of them will be abnormal.
However, in Portugal, as soon as you have a fertilised egg, you are legally not allowed to retrieve more eggs.
This means if I do back to back retrievals, we have to freeze the eggs from the first round and then fertilise them with the eggs harvested from the second round. If we do three retrievals, we have to freeze the eggs from the first 2 rounds and then fertilise them with the eggs retrieved from the 3 round, and so on and so forth. We can do as many retrievals as we like, but as soon as any batch is fertilised, we’re not allowed to do more.
Our options are:
1.) Collect as many eggs as we can from 2 or 3 or 4 rounds, but with the risk that we lose some in the freezing and thawing process. Pro is that we can collect more eggs to fertilise in one shot and hopefully this results in more embryos.
2.) Fertilise the eggs from the first round to reduce risk of egg loss. But that means we have to go through the entire process: fertilise, wait for day 5 embryos, PGTA testing and also transfer (if we make it that far). Only once all the embryos have been used or have failed, can we retrieve again. Given the attrition rate, it seems unlikely the first round will produce anything.
Currently, I am leaning towards collecting as many eggs as possible in 3 to 4 rounds. But a lot of people are saying that egg freezing at my age is too risky – that the eggs are too fragile.
What is your opinion on this? Thanks so much
Author
Answer:
I concur. I would collect as many eggs as possible in advance.
“Empowering Choices: Embryo Banking vs. Egg Banking for Fertility Preservation“
Geoffrey Sher MD
It’s crucial for women to make informed decisions about preserving their fertility. Delaying trying to conceive, relying on egg freezing, or assuming the biological clock can be paused are misconceptions. As women age, egg quality declines, affecting the chance of a successful, healthy pregnancy.
Let’s break down the key points:
- Age and Egg Quality: As women progress past their mid-thirties, the quality of their eggs declines rapidly. This impacts conception rates, leading to higher miscarriage and chromosomal abnormalities like Down syndrome.
- Comparing Chances:
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- At 30, the natural conception rate is around 15-20%, with a 10-15% miscarriage rate and a 1:1000 chance of Down syndrome.
- At 45, natural conception drops to 1-2%, with a 50-60% miscarriage rate and a 1:40 chance of Down syndrome.
- IVF and Age:
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- IVF success rates are better at younger ages, with a 50-60% conception rate for 30-year-olds and a 3-5% chance for 45-year-olds.
- However, IVF doesn’t eliminate the increased risk of miscarriage or chromosomal abnormalities as women age.
- IVF Realities:
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- The success of IVF dramatically decreases with age, making informed decisions crucial.
Preimplantation Genetic Screening (PGS)/Preimplantation Genetic Testing for aneuploidy (PGT-A) is a breakthrough in fertility treatment, aiding the selection of the most viable embryos for a successful pregnancy. By analyzing all chromosomes, it significantly boosts the success rates of IVF. PGS/PGT-A not only increases the chance of a healthy baby per embryo transfer but also reduces the risks of miscarriages and chromosomal birth defects, regardless of the woman’s age.
Who Benefits from PGS/PGT-A?
PGS/PGT-A) has revolutionized embryo evaluation, especially for those facing unexplained IVF failure, infertility, recurrent pregnancy loss (RPL), and older women with diminished ovarian reserve (DOR).
Empowering Older Women: Embryo Banking
PGS/PGT-A is especially beneficial for women over 39 years of age and those with DOR, as it allows the storage (banking) of healthy embryos over multiple cycles, countering the ticking biological clock.. Selective banking of PGS-normal embryos over multiple cycles is a game-changer. It minimizes the impact of age on egg quality, giving these women a chance to make the most of their remaining time to conceive a healthy baby.
Egg Freezing: Factors to Consider
Eggs are vulnerable cells, and freezing a single egg is less effective than freezing a multi-cellular embryo. Additionally, a significant portion of eggs (especially in older women) have chromosomal abnormalities. This makes egg freezing less efficient and embryo freezing, far more successful, especially when selectively freezing PGS/PGT-A-normal blastocysts.
Choosing the Right Path
Importantly, considering the decline in reproductive potential with age, it’s essential for women and couples to explore their fertility options before the age of 35. An aggressive approach, like moving to assisted reproduction and IVF can significantly improve outcomes. For younger women (<35y) who have normal egg reserves, especially those who are not married, have not as yet settled on la “permanent” male partner or a do not feel secure with their existing male partner fathering a child with them might preferentially choose egg freezing . Conversely, women who are comfortable with a designated male partner, older women and those who have DOR might rather select embryo banking.
In the choice between egg and embryo freezing, caution is advised. Current methods for egg selection lack chromosomal analysis. Conversely the performance of PGSGT-A allows for identification of the healthiest embryos for subsequent FET..
Either way, “timing” is a very important consideration.
By understanding these options, you can make an informed decision to maximize your chances of a healthy, happy family. Remember, knowledge is power in the journey to parenthood.
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Herewith are online links to 2 E-books recently co-authored with my partner at SFS-NY (Drew Tortoriello MD)……. for your reading pleasure:
- From In Vitro Fertilization to Family: A Journey with Sher Fertility Solutions (SFS) ; https://sherfertilitysolutions.com/sher-fertility-solutions-ebook.pdf
- Recurrent Pregnancy Loss and Unexplained IVF Failure: The Immunologic Link ;https://drive.google.com/file/d/1iYKz-EkAjMqwMa1ZcufIloRdxnAfDH8L/view
I invite you to visit my very recently launched “Podcast”, “HAVE A BABY” on RUMBLE; https://rumble.com/c/c-3304480
If you are interested in having an online consultation with me, please contact my assistant, Patti Converse at 702-533-2691 or email her at concierge@sherivf.com\