What can I do in 90 days before retrieval?

Direct Answer

What can I actually do in the 90 days before my next IVF retrieval to meaningfully support my egg quality? The 90 days before retrieval cover the full arc of egg maturation from the preantral follicle stage through final oocyte preparation. Targeted supplementation, metabolic stability, toxin reduction, and nervous system support implemented at the start of that window change the biological environment that your eggs are developing inside.

Heather Kish

Heather Kish

Founder, Harvest Health with Heather · Creator, The Egg Awakening™

Best Move

Start CoQ10 (400–600 mg ubiquinol), omega-3 (1,000–2,000 mg EPA + DHA), and protein-first meal composition 90 days before your target retrieval date.

Why It Works

CoQ10 directly supports the mitochondrial ATP production eggs need for chromosome segregation. Omega-3s are incorporated into the oocyte membrane. Protein-first eating flattens the glucose curve that drives the oxidative stress and androgen excess that impair follicular development.

Next Step

Count back 90 days from your expected retrieval date and mark that date as the start of your preparation window. If retrieval is less than 90 days away, start today.

What you need to know

What does the 90-day window actually cover biologically?

The 90-day egg maturation window covers three biologically distinct phases, each with different sensitivities to nutritional, environmental, and metabolic inputs.

Phase 1: Preantral development (days 1–65). Primordial follicles are recruited into the growing pool and begin the slow process of follicle development that is largely independent of FSH stimulation. During this phase, the follicle is establishing its mitochondrial complement, accumulating the cellular machinery that will power chromosome segregation at fertilization. Mitochondrial support (CoQ10, alpha-lipoic acid) and toxin reduction are most relevant at this stage.

Phase 2: Antral/FSH-dependent growth (days 65–80). Follicles enter the antral stage and begin responding to FSH. Granulosa cells proliferate, produce estradiol, and create the follicular fluid environment that surrounds the developing oocyte. The follicular fluid composition at this stage, including its oxidative stress load, inflammatory cytokine content, and nutrient density, is influenced by what the body has been experiencing across the preceding two months.

Phase 3: Final maturation (days 80–90). The IVF stimulation protocol primarily accelerates and synchronizes this final phase. The egg that reaches retrieval has been maturing for the preceding 90 days. Ovarian stimulation does not improve egg quality; it recruits the eggs already maturing. Their quality reflects the environment they have been developing in since day 1 of the window.

This is why beginning a preparation protocol 90 days before retrieval is categorically different from beginning it at the start of stimulation.

Which supplements have the strongest evidence for pre-retrieval egg quality?

CoQ10 has the strongest and most replicated evidence for egg quality in IVF populations. Ubiquinol (the reduced, bioavailable form) at 400–800 mg per day is the studied form and dose.

Evidence summary for key supplements:

  • CoQ10 (ubiquinol, 400–800 mg): Multiple RCTs demonstrate improvements in fertilization rates, blastocyst development, and clinical pregnancy rates in poor responders and women over 35. Mechanism: supports mitochondrial ATP production and functions as an antioxidant in follicular fluid.
  • Omega-3 fatty acids (1,000–2,000 mg EPA + DHA): Incorporated into oocyte membranes; associated with improved blastocyst quality and reduced time to pregnancy in prospective studies. Mechanism: provides structural phospholipids for oocyte membrane fluidity required at fertilization.
  • Vitamin D (dose based on serum level): Women with serum vitamin D above 30 ng/mL have significantly higher live birth rates in IVF meta-analyses. Test serum level before dosing; repletion to 50–80 ng/mL is the target.
  • Melatonin (3 mg at night): Melatonin is produced by granulosa cells in follicular fluid and functions as an antioxidant inside the follicle. Two RCTs in Japanese IVF populations found that 3 mg melatonin nightly beginning 30 days before retrieval improved fertilization rates and reduced follicular oxidative markers. Evidence is promising but less replicated than CoQ10.
  • DHEA (25–75 mg, only if indicated by low androgen markers): Studied in women with DOR, not all IVF patients. Indicated by AMH below 1 ng/mL or low testosterone. Not appropriate as a general pre-retrieval supplement.

What lifestyle factors matter most in the 90-day window?

Three lifestyle factors have direct mechanistic pathways to egg quality that are distinct from supplementation: blood sugar stability, toxin reduction, and sleep quality. Each operates independently and additively.

Blood sugar stability. Postprandial glucose spikes generate reactive oxygen species that accumulate in follicular fluid across the maturation arc. Protein-first meal composition (eating protein before carbohydrates at every meal) reduces postprandial glucose by 25–37 percent. A 10-minute walk after eating activates insulin-independent glucose uptake in muscle. Both are practical, cost-free interventions that reduce the oxidative stress load inside maturing follicles.

Toxin reduction. Phthalates and bisphenols have been detected in follicular fluid and are associated with reduced fertilization rates and blastocyst development. A three-day personal care product swap (fragrance-free, paraben-free alternatives) reduces urinary phthalate and paraben metabolites by 27–45 percent. Replacing the primary cookware source of PFAS and switching to filtered water covers the largest remaining daily exposure sources. A targeted 4–6 week reduction protocol is sufficient.

Sleep quality. Melatonin is produced primarily during sleep and is the principal antioxidant present in follicular fluid. A study in Reproductive Biology found that women who slept fewer than seven hours per night had significantly lower fertilization rates in IVF compared to women sleeping seven to eight hours. Protecting a consistent 7–8 hour sleep window during the 90-day preparation period is a direct intervention in follicular melatonin availability.

What should I ask my RE before the next retrieval?

Most reproductive endocrinologists do not routinely discuss pre-retrieval preparation because it falls outside the clinical protocol they manage. Bringing specific questions creates a more productive conversation than a general inquiry about “improving egg quality.”

Questions to raise with your RE:

  • “Can we review my embryology report from the last cycle?” Ask specifically about fertilization rate, Day 3 embryo grades, Day 5 blastocyst conversion rate, and whether any abnormalities were noted. This data tells you which phase of development was limiting and points toward the most relevant interventions.
  • “Would you consider checking my vitamin D and fasting insulin before the next cycle?” These two markers are the most commonly missed nutritional variables with documented IVF outcome associations. Frame the request as wanting to optimize the cycle rather than as a challenge to their protocol.
  • “Is there a reason not to start CoQ10 and omega-3 supplementation in the 90 days before retrieval?” This framing invites the RE to identify any contraindications rather than defend a position. Most REs have no objection to these supplements; they simply do not raise them routinely.
  • “What does the stimulation protocol from last time suggest about where my eggs are struggling?” An experienced RE can read the stimulation response and embryology outcome together to characterize whether the limiting factor is quantity, quality, or both.

You are not asking your RE to endorse a protocol. You are asking for their clinical read on what the prior cycle data suggests and whether there are any contraindications to the preparation steps you are considering.

How do I know if my 90-day preparation is working?

The most direct confirmation comes from comparing embryology data between cycles, which requires completing the next retrieval. In the meantime, intermediate markers tell you whether the biological systems most relevant to egg quality are moving in the right direction.

Lab markers to retest at 8–12 weeks into the preparation window:

  • Serum vitamin D: Should be rising toward 50–80 ng/mL if you were deficient and supplementing correctly. If levels have not moved after 12 weeks of supplementation, gut absorption of fat-soluble vitamins is the next variable to investigate.
  • Fasting insulin and HOMA-IR: Should be declining toward optimal range (under 8 uIU/mL and under 1.5 respectively) if dietary and exercise interventions are working.
  • Hs-CRP (high-sensitivity C-reactive protein): A systemic inflammatory marker. A decline from elevated baseline (above 1.0 mg/L) after 8–12 weeks of anti-inflammatory interventions confirms that the inflammatory load on the follicular environment is reducing.

Cycle-level markers that track in real time:

  • Luteal phase length extending toward 12–14 days suggests improving progesterone output
  • Mid-luteal progesterone rising toward above 10 ng/mL confirms improving corpus luteum function
  • Reduced premenstrual symptom severity reflects improving hormonal balance

None of these intermediate markers guarantees an improved retrieval outcome. But they confirm that the physiological systems most relevant to egg quality are moving in the target direction before you reach retrieval day.

The The Fertility Intelligence Hub Perspective

When I went into my successful IVF cycle at 44, I had spent 90 days doing exactly what I am describing here: targeted supplementation, stable blood sugar, sleep protected as a non-negotiable, and a systematic reduction of the environmental inputs I could control. I did not know with certainty that it would work. But I knew I was giving those eggs the most supportive internal environment I could build.

What I want women to understand is that the 90-day window is the only leverage point you have. Your RE manages the stimulation protocol. You manage everything that happens in the 90 days before stimulation starts. Those are different jurisdictions, and both matter.

Inside The Egg Awakening, the 90-day preparation framework is built around what the research actually supports, not what feels comprehensive or reassuring. CoQ10 and omega-3s are in because the RCT data is there. Melatonin is in because the follicular fluid antioxidant mechanism is well-characterized. Blood sugar stability is in because the oxidative stress pathway is direct and the interventions are practical. We are not doing a comprehensive protocol; we are doing the evidence-based protocol, implemented consistently across the full maturation window.

Start 90 days out. That window is always running, and earlier is always better.

More questions about this topic

Is 90 days always necessary, or can I start closer to retrieval?

Starting closer to retrieval is better than not starting at all, but the biological benefit diminishes with a compressed window. Interventions begun 30 days before retrieval affect only the cohort entering its final maturation phase. The eggs stimulated in that retrieval cycle began their full maturation arc 90 days earlier. Earlier is always better; starting at 60 days covers the antral and final maturation phases; starting at 90 days covers all three phases.

Should I tell my RE what supplements I am taking?

Yes. Your RE should know your full supplement list before beginning stimulation. Most standard pre-retrieval supplements (CoQ10, omega-3, vitamin D, prenatal) have no known interactions with IVF medications. DHEA is the exception and should be discussed directly with your RE before use, as it can affect stimulation protocols. Melatonin at low doses (3 mg) is generally well-tolerated but worth disclosing.

Can these interventions help even if my AMH is very low?

Yes. The 90-day preparation framework addresses egg quality, not egg quantity. AMH reflects the size of the follicle pool, not the developmental quality of the eggs within it. Women with low AMH who retrieve fewer eggs still benefit from the follicles they do recruit developing in a better-supported mitochondrial and follicular environment. Fewer eggs with higher quality per egg can produce better clinical outcomes than more eggs at lower quality.

What if my clinic does not support this kind of preparation?

Most IVF clinics do not actively support or discuss pre-retrieval preparation because it falls outside their clinical protocol scope. They also rarely object when patients raise it. The most practical approach: implement the preparation protocol independently, inform your RE of what you are taking, and ask specifically whether anything on your list is contraindicated for your upcoming cycle. A reasonable RE will engage with that conversation.

How do I stay calm and hopeful through a 90-day preparation without becoming obsessive?

Set the protocol once, implement it, and treat it as done rather than as something to continuously optimize. The 90-day window contains a protocol, not a project. Continuous research, supplementation revision, or tracking beyond the recommended lab retests turns preparation into hypervigilance, which generates cortisol at the expense of the hormonal balance you are working to support. Do the work, then release the outcome.

Related pages

Heather Kish

Heather Kish

Heather Kish is the founder of Harvest Health with Heather and the creator of The Egg Awakening, a 90-day root-cause fertility coaching program. After four years of her own unexplained infertility, multiple pregnancy losses, and fibroids, she built a root-cause approach combining nutrition, nervous-system regulation, and egg health support. She conceived via IVF at 44 and now helps other women find answers faster and suffer less.

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