Understanding IMSI Treatment
Learn from our experts and get inspired by real patient journeys
You received a blood test result. The number was low — lower than the reference range — and whoever explained it to you may have used words like ‘diminished reserve’, ‘difficult to achieve pregnancy’, or perhaps even suggested that using someone else’s eggs is your only option.
We want to say something clearly, at the very start of this page: a low AMH result is not a verdict. It is a measurement. It tells us about the number of eggs remaining in your ovaries — it does not tell us about the quality of those eggs, and it does not tell us that pregnancy with your own eggs is impossible.
At Wellspring IVF & Women’s Hospital in Ahmedabad, our approach to low AMH is built around a single, non-negotiable principle: we try with your own eggs first. We use the most advanced stimulation protocols available for poor responders, we maximise every cycle with techniques like Dual Stimulation and Embryo Banking, and we give your own biology every genuine opportunity before any alternative is considered.
“In my 15 years of treating fertility patients, the cases I find most rewarding are the women who arrive having been told their AMH is ‘too low’ for IVF. Low AMH is one of the most misunderstood reports in fertility medicine. A low number does not mean poor- quality eggs. I have seen women with AMH of 0.3 ng/mL achieve successful pregnancies with their own eggs through careful, personalised protocols. The answer is never to give up on your own eggs without a genuine effort.” — Dr. Pranay Shah, MS (ObGy), Director, Wellspring IVF & Women’s Hospital
Anti-Müllerian Hormone (AMH) is a protein hormone produced by the small follicles in the ovaries. Because these follicles contain the eggs that will eventually be recruited for ovulation, the level of AMH in the blood gives us an indirect measurement of how many eggs remain in the ovarian reserve — what fertility specialists call the ‘ovarian reserve.’
AMH is one of the most useful fertility blood tests because, unlike FSH or oestrogen, it does not fluctuate significantly during the menstrual cycle. This means it can be tested on any day of your cycle and gives a consistent, reliable picture of your remaining egg quantity.




| Category | AMH Level (ng/mL) | Fertility Implication |
|---|---|---|
| Optimal | Above 2.0 | Good egg reserve. Responds well to IVF stimulation. |
| Normal | 1.0 – 2.0 | Adequate reserve for IVF. Most patients respond well. |
| Low | 0.5 – 1.0 | Reduced reserve. Specialised IVF protocols recommended. Many successes possible. |
| Very Low | Below 0.5 | Significantly diminished reserve. Advanced poor-responder protocols required. Own eggs attempted first. |
This is the most critical distinction in low AMH management, and one that is frequently misunderstood — even by some clinicians.
AMH tells us how many eggs you have remaining. It does not tell us about the genetic quality or developmental potential of those eggs. A woman with AMH of 0.4 ng/mL may have 3–4 eggs retrieved in an IVF cycle — but if those eggs fertilise normally and develop into good-quality embryos, the success rate per embryo transferred is not significantly different from a woman with a higher AMH.
The challenge with low AMH is not egg quality — it is egg quantity per cycle. Fewer eggs means fewer chances per stimulation. This is precisely why our advanced protocols (Dual Stimulation and Embryo Banking) exist: to maximise the total number of eggs collected, cycle by cycle, until we have enough good-quality embryos to attempt transfer.
Low AMH can result from several different factors. Understanding the underlying cause matters, because it may influence the treatment approach:
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When a woman with low AMH comes to Wellspring IVF, the onversation does not begin with donor eggs. It begins with a thorough assessment of what her ovaries are genuinely capable of — and then with a protocol specifically designed to maximise that capability.
Dr. Pranay Shah has developed a structured approach for poor esponders that is used before any discussion of alternative options. This approach has two defining techniques:
Dual Stimulation is one of the most significant advances in fertility treatment for poor responders in the past decade. It is based on a scientific observation: follicles do not grow only in the follicular phase of the cycle (days 1–14). The ovary can be stimulated to produce
additional eggs in the luteal phase (days 15–28) of the same cycle.
In a standard IVF cycle, stimulation is performed once — typically in the follicular phase. For a woman with low AMH who produces only 1–2 eggs in a standard cycle, this provides very limited material for embryo development.
In a DuoStim cycle, we stimulate twice:
The result: in a single calendar month, we may collect double the number of eggs compared to a conventional single-stimulation cycle. For a poor responder, this can mean the difference between having 1–2 embryos and having 4–5 — a significant increase in the
cumulative probability of a successful pregnancy.
Current evidence shows that luteal phase-derived eggs have comparable fertilisation rates and embryo quality to follicular phase eggs. There is no compromise on quality — we are simply using a biological window that was previously left unexploited.
Protocol 2: Embryo Banking — Accumulating Your Best Chances
Embryo Banking (also called Embryo Accumulation) is a strategy where, rather than attempting an embryo transfer after every stimulation cycle, we vitrify (freeze) all embryos obtained across multiple cycles and accumulate them into a single cohort before any
transfer is attempted.
The logic is straightforward: for a woman with low AMH who produces 1–2 eggs per cycle, a single cycle may not yield enough embryos to achieve a transfer. But if we perform 2–3 stimulation cycles — often using DuoStim to maximise each month — and bank all the resulting blastocysts, we may accumulate 4–6 high-quality frozen embryos.
We then perform a single Frozen Embryo Transfer (FET) cycle in a well-prepared uterine environment, choosing the best embryo from the banked cohort. This strategy improves outcomes in several ways:
At Wellspring IVF, Dr. Pranay Shah carefully counsels each patient on whether DuoStim, Embryo Banking, or a combination of both is the most appropriate strategy for their specific AMH level, age, antral follicle count, and previous response history.
Beyond Dual Stimulation and Embryo Banking, Dr. Shah uses a comprehensive set of evidence-based interventions for women with low AMH:
For the overwhelming majority of women with low AMH, the strategies above provide a genuine and often successful path to pregnancy with their own eggs. However, we believe in honest, transparent counselling — and there are situations where, after an exhaustive and genuine attempt with own eggs, the likelihood of success becomes very low.
In such circumstances, Dr. Shah will have a full, unhurried conversation about the remaining pathways. At Wellspring IVF, this conversation is always factual, never pressured, and always led by what is in your best interest — not by commercial considerations.
Donor Egg IVF — Important Information Under the ART (Regulation) Act, 2022
In India, the use of donor eggs in assisted reproduction is strictly regulated by the Assisted Reproductive Technology (Regulation) Act, 2022, and the rules framed thereunder. At Wellspring IVF, we follow these regulations completely and without exception.
Under the ART Act 2022, oocyte (egg) donation is permitted only through a registered ART Bank. Key provisions that patients must understand:
We understand that reaching this conversation is emotionally significant. Dr. Shah and our counselling team will guide you through every aspect of this process — the medical procedure, the legal framework, the emotional considerations, and the realistic success rates — with complete transparency and compassion.
Low AMH sometimes occurs alongside other fertility conditions. A complete evaluation at Wellspring IVF ensures nothing is overlooked:
Yes — low AMH reduces the probability of natural conception because there are fewer follicles recruited each cycle, meaning the chance of spontaneous ovulation producing a viable egg in any given month is lower. However, it does not make natural conception impossible. Many women with AMH below 1.0 ng/mL conceive naturally. The key factors are age, egg quality, partner’s sperm parameters, and tubal health.
No — this is the most important misconception to address. AMH measures the quantity of your remaining follicles, not the genetic or developmental quality of your eggs. A woman with low AMH can have excellent-quality eggs. Egg quality declines with age, but this is a separate biological process from the decline in AMH. Two women aged 32 with the same low AMH level will typically have similar egg quality. The challenge is the smaller number of eggs available per cycle.
Dual Stimulation involves two separate ovarian stimulations within a single menstrual cycle — one in the follicular phase and one in the luteal phase. It is well-supported by clinical evidence published in peer-reviewed reproductive medicine journals. Current data shows that luteal phase oocytes have comparable fertilisation rates and embryo developmental competence to follicular phase oocytes. The approach is considered safe and is specifically designed for poor responders who need to maximise egg yield per month.
This varies significantly based on your specific AMH level, age, antral follicle count, and how your ovaries respond to stimulation. Some patients accumulate enough embryos in a single DuoStim cycle. Others benefit from 2–3 banking cycles before transfer. Dr. Shah will discuss a realistic expectation at your first consultation based on your complete diagnostic picture — not a one-size-fits-all estimate.
DHEA supplementation has a growing body of evidence supporting its use in diminished ovarian reserve. Several randomised controlled trials and meta-analyses have reported improved ovarian response, higher egg yields, and better embryo quality in poor responders who supplement with DHEA for 6–12 weeks before IVF. It is not effective for every patient, and Dr. Shah prescribes it selectively based on individual assessment rather than as a blanket recommendation.
There is no absolute threshold, but the general principle is this: time is a significant factor in low AMH. Since the ovarian reserve continues to decline, delay can be costly. Women under 35 with AMH between 0.5–1.0 ng/mL may have 6–12 months to attempt natural conception before pursuing IVF, depending on other factors. Women over 35, or with AMH below 0.5 ng/mL, are generally advised to pursue IVF without significant delay. Dr. Shah will give you a personalised recommendation at consultation.
Unfortunately, some fertility centres use AMH thresholds as a reason to decline treatment with own eggs. At Wellspring IVF, we do not operate this way. We evaluate every patient individually, consider the complete clinical picture, and offer a genuine trial with own eggs using our advanced protocols before any alternative is discussed. Many of our most rewarding outcomes are in patients who were told elsewhere that their situation was hopeless.