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New Model Reveals Why Single Births Predominate in Human Pregnancies

April 22, 2026
in Biology
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New Model Reveals Why Single Births Predominate in Human Pregnancies
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Each month, the intricate orchestration of a woman’s menstrual cycle begins within the ovary, where a cohort of 10 to 20 antral follicles—fluid-filled sacs enclosing immature eggs—undergo preparation for potential maturation. However, the biological choreography is highly selective; in the vast majority of cycles, only one follicle is chosen to mature fully, culminating in the release of a single egg primed for fertilization. Natural occurrences of fraternal twins, resulting from the simultaneous release of two eggs, remain relatively rare, constituting roughly 2-3% of pregnancies. This biological precision in follicle selection has long piqued scientific curiosity: what governs the seemingly exclusive choice of a single dominant follicle each cycle?

Anatoly Kolomeisky, a chemistry professor at Rice University with extensive expertise in physical chemistry, embarked on an investigative journey to unravel this question. Familiar with the complexities of molecular interactions, Kolomeisky turned to a fresh perspective, analyzing hormonal data through the lens of chemical process modeling. Two hormones, follicle stimulating hormone (FSH) and estradiol, have long been implicated in follicle physiology, but the exact interplay dictating follicular dominance had evaded clear elucidation. Conventional hypotheses emphasized factors such as follicle size or differential hormonal sensitivity as deterministic criteria for selection. However, Kolomeisky’s approach leveraged rigorous computational simulation and stochastic modeling to challenge these traditional paradigms.

Published in the Journal of The Royal Society Interface, this innovative research countryside the follicle selection mechanism as inherently stochastic rather than deterministic. In essence, the model posits that selection is a random event governed by probabilistic dynamics rather than the hierarchical superiority of one follicle’s physiological attributes over another. This finding disrupts prior assumptions and opens new avenues to comprehend how such randomness achieves biological precision.

The study delineates the follicular phase of the menstrual cycle as a critical window where follicle stimulating hormone (FSH) concentrations rise gradually. Once FSH levels reach a defined biochemical threshold, the model predicts that any one of the pre-prepared follicles can be randomly selected to undergo full maturation. Following selection, the developing follicle secretes estradiol, a steroid hormone that exerts a negative feedback effect on FSH, rapidly reducing its concentration below the threshold necessary for further selections. This feedback loop functions as a biological gatekeeper, effectively preventing additional follicles from reaching maturity within the same cycle.

This FSH-estradiol regulatory axis is crucial: it underpins not only the randomness of follicle selection but also ensures the exclusivity of the dominant follicle. The rapid decline of FSH after the initial follicular selection introduces a narrow temporal window during which the maturation trigger is active, drastically limiting the window of opportunity for multiple follicle selection. Consequently, this stochastic yet finely tuned mechanism preserves both randomness and precision.

One of the most intriguing aspects of the model lies in its explanation for rare occurrences when two follicles mature simultaneously. Such events likely result from the stochastic dynamics intersecting with subtle shifts in the timing or amplitude of hormone fluctuations around the threshold. Small variations in the tempo of FSH decline or estradiol rise can allow for a secondary follicle to be selected before FSH falls too low. This provides a scientifically coherent framework for understanding fraternal twinning and shortens the explanatory gap that deterministic models struggled to address.

The implications of this stochastic model extend beyond normal physiology and reach into the realm of reproductive health challenges. For example, as women age, regulatory mechanisms around the FSH-estradiol feedback loop may experience subtle loosenings, increasing the probability of dual follicle selection and thus the incidence of fraternal twins in older women. This scenario aligns with epidemiological data indicating higher twinning rates in women over 35, offering a mechanistic hypothesis grounded in hormone dynamics.

Moreover, conditions such as polycystic ovary syndrome (PCOS) can potentially be reframed through this model’s insights. PCOS patients commonly exhibit low circulating FSH levels, which according to the model may never surpass the critical threshold needed to initiate follicle selection. This hormonal insufficiency could underlie the follicular arrest and anovulation frequently observed in PCOS, suggesting new therapeutic targets that modulate the FSH threshold dynamics.

The strength of this research rests in its computational sophistication and reliance on robust data alignment. By constructing a mathematical framework that integrates biochemical feedbacks with stochastic processes, the model transcends simplistic linear causality and embraces the inherent complexity of ovarian physiology. This methodology not only aligns with empirical hormone concentration data but also offers predictive power to explore physiological and pathological scenarios within reproductive endocrinology.

In addition to elucidating the fundamental science, this research underscores the value of interdisciplinary approaches, where chemical kinetics and probabilistic modeling intersect with reproductive biology to uncover novel explanatory models. It illustrates a paradigm where biological processes traditionally thought to be deterministic may instead operate through finely tuned random mechanisms, challenging long-standing dogmas and informing future experimental designs.

Future exploration emerging from this model will likely delve deeper into quantifying the precise feedback kinetics and exploring individual variability in hormonal thresholds, potentially incorporating genetic and environmental modifiers. Understanding how different physiological states or interventions affect this stochastic mechanism could revolutionize fertility treatments and improve reproductive health management.

Kolomeisky’s team’s contributions demonstrate how theoretical modeling can illuminate the intricate dance of hormones governing the menstrual cycle and follicular selection. Their work reveals a hidden simplicity in apparent biological complexity, wherein a controlled randomness yields consistent outcomes crucial for human reproduction—a testament to the elegance of biological systems shaped by chance and control.

As we continue to decode the mechanisms underpinning follicle selection, this stochastic model stands as a landmark, not only redefining fundamental reproductive biology but also offering pragmatic pathways to address infertility, hormonal disorders, and age-related fertility changes. The interplay of FSH and estradiol emerges as a finely tuned stochastic relay, orchestrating the critical selection of the dominant follicle with remarkable precision amidst inherent biological variability.

Subject of Research:
Follicle selection mechanisms during the menstrual cycle, focusing on the interplay between follicle stimulating hormone and estradiol, through computational modeling.

Article Title:
Stochastic mechanism of dominant follicle selection: selection of one suppresses selection of others

News Publication Date:
22-Apr-2026

Web References:
http://dx.doi.org/10.1098/rsif.2025.0915

Image Credits:
Zhuoyan Lyu/Rice University

Keywords:
Follicle selection, follicle stimulating hormone, estradiol, menstrual cycle, ovarian physiology, stochastic modeling, follicular phase, reproductive biology, fraternal twins, polycystic ovary syndrome, hormonal feedback, computational simulation

Tags: chemical process modeling in biologydominant follicle mechanismestradiol hormone effectsfollicle selection processfollicle stimulating hormone rolesfraternal twin pregnancy rateshormonal regulation of ovulationhuman pregnancy biologymenstrual cycle hormonesovarian follicle developmentreproductive physiology researchsingle egg maturation
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