Chemical Biology: In-Depth Description

Chemical Biology is the scientific discipline spanning the fields of chemistry and biology, fundamentally defined by the application of chemical techniques, analytical methods, and synthetically derived small molecules to the study and manipulation of biological systems. Unlike classical biochemistry, which typically focuses on studying the innate chemistry of biological molecules within their natural environments, chemical biology actively intervenes. It utilizes rationally designed chemical tools to perturb, probe, and ultimately understand biological processes at a molecular and mechanistic level. The primary goals of this field include unraveling complex cellular signaling pathways, identifying novel therapeutic drug targets, and engineering innovative molecular tools that can interface seamlessly with living systems in real-time.

AI outperforms doctors at summarizing complex cancer pathology reports

Study authors Drs. Mohamed Abazeed (right), Yirong Liu and Troy Teo (left) demonstrates a prototype AI tool that summarizes cancer pathology reports, shown here in a radiation oncology setting.
Photo Credit: Northwestern University

Scientific Frontline: Extended "At a Glance" Summary: AI Summarization of Cancer Pathology Reports

The Core Concept: Open-source artificial intelligence models can generate more comprehensive and structured summaries of complex cancer pathology reports compared to physician-written versions.

Key Distinction/Mechanism: Unlike manual summarization, which is subject to time constraints and cognitive overload, these AI systems analyze extensive longitudinal data to consistently capture critical microscopic, immunohistochemical, and molecular findings. The AI serves as an augmentative tool to support clinical decision-making and ensure no vital genetic details are overlooked.

Origin/History: A Northwestern Medicine study published in April 2026 evaluated 94 de-identified lung cancer pathology reports to assess the efficacy of large language models in a clinical oncology setting.

Major Frameworks/Components:

• Open-Source Large Language Models (LLMs): Utilization of models that can be run locally to protect patient privacy, specifically Meta's Llama (3.0, 3.1, 3.2), Google's Gemma 9B, Mistral 7.2B, and DeepSeek-R1.
• Histopathological Analysis: Extraction and synthesis of microscopic tumor characteristics.
• Immunohistochemical Evaluation: Processing of protein expression testing results.
• Genomic and Molecular Data Processing: Reliable identification of actionable genetic markers critical for targeted cancer therapies.

Nematodes show how lack of food shapes the next generation

Two nematodes (C. elegans) with eggs and hatched larvae. Red coloring shows the protein factories of the cells (ribosomes), and the light areas mark the reproductive organs (gonads).
Image Credit: © Courtesy of B. Towbin

Scientific Frontline: Extended "At a Glance" Summary: Non-Genetic Inheritance of Ribosomes in Nematodes

The Core Concept: The nutritional environment of mother nematodes directly dictates the early growth rate of their offspring by determining the quantity of ribosomes—cellular "protein factories"—passed down through the egg. If the maternal food supply is restricted, the offspring inherit fewer ribosomes, resulting in slower initial development.

Key Distinction/Mechanism: Unlike genetic inheritance, which relies on DNA alteration, this represents a direct, non-genetic transmission of physical cellular machinery. The process is governed by the mTORC1 signaling pathway in the mother, which directly curtails the deposition of ribosomes into eggs during periods of starvation. This straightforward mechanism bypasses the need for the offspring to develop complex, reactive molecular pathways to adapt to their inherited environment.

Origin/History: This discovery was published in PLOS Biology in April 2026, stemming from collaborative research led by Prof. Dr. Benjamin Towbin at the University of Bern's Institute of Cell Biology alongside the Centre for Genomic Regulation in Barcelona.

How bacteria suppress immune defenses in stubborn wound infections

Experiments found that wounds infected with E. faecalis (seen here) had dampened immunity, allowing E. faecalis to persist and enabling co-infecting bacteria like E. coli to thrive. A mouse model allowed researchers to study how lactic‑acid‑driven immune suppression promotes persistent, polymicrobial infections.
Image Credit: Janice Haney Carr / Centers for Disease Control and Prevention

Scientific Frontline: Extended "At a Glance" Summary: Bacterial Immune Suppression in Chronic Wounds

The Core Concept: Enterococcus faecalis (E. faecalis) is a highly resilient bacterium that suppresses the body’s initial immune defenses in wounds by releasing large amounts of lactic acid. This localized acidification deactivates key immune cells, allowing E. faecalis and other co-infecting microbes to establish persistent, hard-to-treat infections.

Key Distinction/Mechanism: Unlike bacteria that simply resist antibiotics, E. faecalis actively sabotages the host immune system through a targeted, two-step mechanism. The secreted lactic acid enters macrophages via the MCT-1 lactate transporter and simultaneously binds to the GPR81 lactate-sensing surface receptor. Engaging both pathways effectively shuts down the macrophage's downstream inflammatory response by preventing the activation of NF-κB, a critical intracellular immune alarm signal.

Major Frameworks/Components:

• Microenvironmental Acidification: The use of bacterial lactic acid to actively lower wound pH and alter the local tissue environment.
• Macrophage Deactivation: The direct targeting and suppression of the primary immune cells responsible for initiating the clearance of pathogens.
• Receptor-Mediated Silencing: The specific engagement of MCT-1 and GPR81 pathways to block intracellular immune signaling.
• NF-κB Inhibition: The molecular silencing of the host's fundamental "danger" alarm network.
• Polymicrobial Facilitation: The cascade effect wherein the dampened localized immunity creates an opportunistic environment for secondary pathogens, such as Escherichia coli, to rapidly colonize and proliferate.

Scientists discover how key immune cells protect the prostate

Confocal microscopy of murine prostates at 7 (left), 30 (center) and 250 (right) days post infection. Colors indicated and scale bar shown. E-Cadherin (red) marks epithelial tissue, CD45.1 (green) identifies T cells specific to the infection and nuclei are shown in blue (DAPI).
Image Credit: Kianoosh Mempel

Scientific Frontline: Extended "At a Glance" Summary: Tissue-Resident Memory T Cells in the Prostate

The Core Concept: The discovery that specific immune cells, known as tissue-resident memory T cells, migrate to and establish long-term residency within the prostate to guard against infections and potentially combat disease.

Key Distinction/Mechanism: Previous models suggested the prostate was largely immunologically inaccessible, as T cells often struggle to infiltrate prostate tumors. This research demonstrates that the prostate actually functions as a vital immunological barrier tissue. Following an infection, memory T cells are deployed to the prostate where they adapt to the local tissue environment, remaining there for months or years to provide continuous, localized defense.

Major Frameworks/Components:

• Spatial Immunology: The application of advanced mapping techniques to identify the exact physical arrangement and specific niches of immune cells within prostate tissue.
• Single-Cell Technologies: Analytical tools utilized to track cellular activity, differentiation, and the evolution of T cell responses over time in both viral mouse models and healthy human tissue samples.
• Barrier Tissue Paradigm: The functional reframing of the prostate from a strictly reproductive organ to a critical immunological barrier protecting the male reproductive system from pathogens utilizing the shared urethral tract.

Aerobiology:In-Depth Description

Aerobiology is the scientific study of airborne biological particles, focusing on their emission, transport, and deposition in the atmosphere, as well as their interactions with the environment and human health. The primary goal of this field is to understand the life cycle of bioaerosols—which include pollen, fungal spores, bacteria, viruses, microalgae, and tiny arthropods—and to predict their movement and impact on ecosystems, agriculture, and public health.

Bacteriology: In-Depth Description

Bacteriology is the specialized branch of microbiology devoted to the comprehensive study of bacteria, encompassing their morphology, ecology, genetics, and biochemistry. The primary goal of this discipline is to understand the fundamental nature of these single-celled prokaryotic organisms, including their evolutionary mechanisms, their symbiotic or pathogenic relationships with host organisms, and their immense utility in industrial and environmental processes. By isolating, identifying, and characterizing bacterial species, scientists in this field strive to mitigate infectious diseases, harness microbial metabolic pathways for biotechnology, and decipher the critical roles bacteria play in sustaining the Earth's biosphere.

New Sensors Lower the Cost of Studying Genetic Disorders

Photo Credit: Navya Mishra.

Scientific Frontline: Extended "At a Glance" Summary: CAMEO Sensor Technology for Cerebral Organoids

The Core Concept: CAMEO (Conformal Array for Monitoring Electrophysiology of Organoids) is a low-cost, scalable sensor platform designed to monitor electrical activity within human cerebral organoids.

Key Distinction/Mechanism: Unlike traditional, expensive microelectrode arrays that rely on costly materials, CAMEO utilizes 12 flexible carbon nanotube strands arranged in a basket-like structure. This design suspends the organoid and detects low-amplitude electrophysiological signals without the need for specialized workflows or expensive gold electrodes.

Major Frameworks/Components: 

• Human Cerebral Organoids: Millimeter-sized tissues cultured from stem cells that replicate the complexity and specific cell types of human brain regions.
• Carbon Nanotube Microelectrode Arrays (MEAs): Highly sensitive, flexible 3D electrodes capable of recording extracellular electrophysiological activity.
• High-Throughput Processing: A scalable diagnostic approach that allows for simultaneous, multi-sample data collection in standard cell culture plates.

Biophysics: In-Depth Description

Biophysics is an interdisciplinary field of science that applies the principles, theories, and methods of physics to understand how biological systems operate. The primary goal of biophysics is to bridge the gap between the complexity of life and the fundamental laws of nature, mapping out the physical mechanisms that drive biological function from the molecular and subatomic scale to complex ecosystems.

Shields and bodyguards: scientists uncover the hidden defences of a deadly childhood cancer

Neuroblastoma imaging showing cancer cells (white), immune cells (yellow) supportive tissue (blue) and blood vessels (red).
Photo Credit: The University of Queensland.

Scientific Frontline: Extended "At a Glance" Summary: Hidden Defenses in Neuroblastoma

The Core Concept: Researchers have comprehensively mapped the microenvironment of neuroblastoma, a highly lethal pediatric cancer, discovering that the tumors utilize surrounding immune cells as "bodyguards" and specific proteins as "shields" to evade natural cell death.

Key Distinction/Mechanism: Unlike previous methodologies that merely cataloged the cells present in a tumor, this research utilized advanced spatial mapping technology to identify the precise geographical relationship between cancer cells and immune cells. It revealed that high-risk neuroblastoma cells resist ferroptosis—a natural cell death process triggered by toxic lipid accumulation—by expressing a protective shielding protein known as GPX4.

Major Frameworks/Components:

• Spatial Mapping Technology: Employed to construct high-resolution 2D maps of tumor samples from 27 pediatric patients, allowing researchers to observe the exact spatial orientation and interactions of cells, active genes, and proteins.
• Ferroptosis: A specialized form of regulated cell death driven by the toxic buildup of lipid peroxides, which the cancer cells must actively suppress to survive.
• GPX4 Protein: Identified as the molecular "shield" that neutralizes toxic fats, thereby saving the cancer cells from undergoing ferroptosis.
• Microenvironmental "Bodyguards": Specific immune cells strategically positioned within the tumor's architecture that actively protect the cancer cells from the body's natural defenses.

Nature’s photocopiers caught ‘doodling’ – and scientists say it could revolutionise how DNA is written

Nanoscale view of several interwoven fragments of ‘doodled’ DNA (orange and white strands) imaged on a near perfectly flat mica surface (shown in blue) using a custom high-speed atomic force microscope built at the University of Bristol.
Image Credit: Thomas Gorochowski

Scientific Frontline: Extended "At a Glance" Summary: DNA Polymerase "Doodling"

The Core Concept: DNA polymerases—the microscopic biological machines responsible for replicating DNA—possess an innate capability to synthesize entirely new, highly complex, and extensive DNA sequences from scratch without utilizing an existing template.

Key Distinction/Mechanism: Standard DNA replication relies on reading and mirroring an existing DNA strand. Conversely, "doodling" involves the autonomous generation of distinct genetic material ranging from simple two-base repeats to elaborate eight-base motifs. Furthermore, unlike contemporary chemical DNA synthesis, which is slow and limited to sequences of a few hundred bases, this template-free synthesis can generate fragments exceeding 85,000 bases in a single reaction. Crucially, the process can be "steered" by modulating environmental parameters, such as altering the temperature or restricting the available DNA building blocks.

Major Frameworks/Components: 

• Nanopore Sequencing: Utilized to map the full-length structures of thousands of autonomously generated DNA molecules, revealing unprecedented sequence complexity.
• Environmental Modulation: The methodology of altering reaction conditions (e.g., temperature shifts, reagent limitation) to dictate the specific repeating patterns and motifs synthesized by the polymerases.
• AI-Powered Protein Design: Proposed as an integrative framework to optimize and harness these biological machines for advanced, guided synthesis.

Genetically modified marmosets as a model for human deafness

"Myrabello“ is a genetically modified marmoset. The image is from a video.
Photo Credit: Katharina Diederich

Scientific Frontline: Extended "At a Glance" Summary: Genetically Modified Marmosets as a Model for Human Deafness

The Core Concept: Researchers have successfully utilized CRISPR/Cas9 technology to create genetically modified marmosets with a non-functional OTOF gene, establishing the first realistic primate model for congenital human deafness.

Key Distinction/Mechanism: Unlike previous mouse models or cell cultures, this primate model closely mirrors human hearing development and physiology. By precisely knocking out the OTOF gene, the inner ear ceases to produce the protein otoferlin. Without otoferlin, acoustic signals cannot be transmitted from the inner ear's hair cells to the auditory nerve, resulting in profound deafness despite a physically intact ear structure.

Major Frameworks/Components:

• CRISPR/Cas9 Genome Editing: Applied to precisely eliminate the OTOF gene function in fertilized marmoset eggs.
• Reproductive Biology: Involves the successful implantation of the modified embryos into surrogate mothers, resulting in healthy, normally developing offspring that are deaf from birth.
• Electrophysiological Verification: The use of EEG-like diagnostic methods to confirm deafness and cellular analysis to verify the absence of the otoferlin protein.
• Translational Pipeline: Serves as a critical bridge connecting in vitro and murine research to clinical human applications.

Two organs, one brain area: How fish orientate themselves in the water

The brain regions involved in pineal ‘color’ detection
Light is detected by both the eye and the pineal organ. The light-sensitive opsin PP1 in the pineal cells senses the balance of ultraviolet and visible light and converts it into neural signals. These signals are processed in the tegmentum, where they regulate the fish’s up and down swimming behavior.
Image Credit: Osaka Metropolitan University

Scientific Frontline: Extended "At a Glance" Summary: Pineal and Visual Light Integration in Zebrafish

The Core Concept: The tegmentum region in the zebrafish midbrain integrates light signals from both the eyes and the pineal organ (the "third eye") to coordinate spatial orientation. This neural integration allows the fish to adjust its up-and-down swimming behavior based on the specific wavelengths of ambient environmental light.

Key Distinction/Mechanism: Unlike standard vision, which relies exclusively on ocular photoreceptors, this mechanism utilizes the light-sensitive protein opsin parapinopsin 1 (PP1) within the pineal organ to evaluate the balance of ultraviolet (UV) and visible light. The tegmentum processes these pineal signals alongside standard visual inputs from the eyes, prompting the fish to swim upward when UV light is weak and downward when UV light is strong.

Major Frameworks/Components:

• Opsin Parapinopsin 1 (PP1): A specialized photoreceptive protein located in the pineal organ that reacts in contrasting ways to UV and visible light to detect color balance.
• The Pineal Organ: Often referred to as the "third eye," it detects ambient light conditions and transmits non-visual color-detection signals via ganglion cells.
• The Tegmentum: The specific midbrain region responsible for synthesizing input from both the visual system (eyes) and the pineal organ to dictate physical movement.
• Calcium Imaging: A biological visualization technique used on transparent zebrafish larvae to observe calcium level fluctuations, allowing researchers to measure the strength of neural activity and map the active circuits.

Ural Bacteria Will Help Wheat Survive on Devastated Lands

The work of UrFU biologists will help plants adapt to stressful conditions.
Photo Credit: Stepan Dolgov

Scientific Frontline: Extended "At a Glance" Summary: Salinity-Resistant Biofertilizing Bacteria

The Core Concept: Researchers have identified two specific strains of bacteria (AP9 and AP12) capable of entering into a symbiotic relationship with plants to enhance survival, root development, and seedling growth in highly saline soils. These microorganisms function as living biofertilizers that protect crops, such as wheat, from osmotic and ion-specific toxicity.

Key Distinction/Mechanism: Unlike traditional mineral fertilizers (such as synthetic ammonia or nitrates) that provide a static nutrient deposit, these bacterial biofertilizers offer a prolonged, dynamic effect. They continuously synthesize phytohormones and increase nutrient availability throughout the vegetation period. By reducing oxidative stress and increasing the number of primary roots, the bacteria expand the plant's absorbent surface area and improve water and mineral uptake in otherwise hostile, saline environments.

Major Frameworks/Components: 

• Bacterial Strains AP9 and AP12: Halotolerant (salt-tolerant) microorganisms isolated from naturally saline lake ecosystems.
• Symbiotic Phytohormone Synthesis: The continuous production of plant hormones by the bacteria to stimulate crop growth.
• Oxidative Stress Reduction: Biological mitigation of the cellular damage caused by excess salt accumulation.
• Root Architecture Modification: The stimulation of primary root generation to maximize the surface area for efficient nutrient and water absorption.

Human sperm may get lost in space

Image Credit: Scientific Frontline

Scientific Frontline: Extended "At a Glance" Summary: Extraterrestrial Sperm Navigation

The Core Concept: The navigational abilities of human and mammalian sperm, along with early embryonic development, are significantly impaired by the lack of gravity in extraterrestrial environments.

Key Distinction/Mechanism: Microgravity disrupts a sperm's spatial orientation and navigation rather than its physical motility (movement). However, the introduction of the sex hormone progesterone can partially mitigate this disorientation by chemically guiding the sperm toward the site of fertilization, counteracting the effects of zero gravity.

Major Frameworks/Components:

• 3D Clinostat Simulation: Utilizing a specialized machine developed by Firefly Biotech to simulate zero-gravity conditions by rotating cells to disorient them.
• Reproductive Tract Mazes: Laboratory models designed to mimic the physical barriers of the female reproductive channel.
• Progesterone Interventions: Harnessing sex hormones naturally released by the egg as a potential chemical navigation beacon in the absence of gravity.
• Embryogenesis Monitoring: Tracking a 30 percent reduction in successful fertilization rates and cellular development delays caused by prolonged microgravity exposure in animal models.

Mechanobiology: In-Depth Description

Mechanobiology is an interdisciplinary field of science that investigates how physical forces and alterations in the mechanical properties of cells and tissues influence cellular behavior, development, physiology, and disease. Its primary goal is to understand the precise mechanisms by which biological systems sense, generate, and respond to physical cues—a process known as mechanotransduction—and how these physical inputs are integrated with genetic and biochemical pathways to maintain biological homeostasis or drive pathological states.

How inflammation may prime the gut for cancer

An image of mouse colon during chronic colitis displays the effects of inflammation, which can lead to lasting changes in the epigenome that promote cancer.
Image Credit: Courtesy of the Buenrostro Lab 

Scientific Frontline: Extended "At a Glance" Summary: Epigenetic Priming of Colorectal Cancer

The Core Concept: Chronic intestinal inflammation leaves lasting molecular scars, or epigenetic "memories," on seemingly healed gut tissues, fundamentally priming these healthy-appearing cells for future cancer development.

Key Distinction/Mechanism: Unlike traditional models that attribute tumorigenesis solely to the gradual accumulation of genetic mutations, this discovery highlights a structural "one-two punch" mechanism. Prior bouts of inflammation alter the cell's epigenome by keeping specific cancer-associated DNA sites open and accessible. If a subsequent oncogenic mutation occurs later in life, the cell exploits these pre-opened genomic regions to rapidly activate cancer-driving genes and accelerate tumor growth.

Major Frameworks/Components:

• Multiplexed Single-Cell Profiling: An advanced analytical method developed to simultaneously measure individual cells' transcriptional states (active gene expression), epigenomic states (chromatin accessibility), and clonal histories (cellular family trees).
• Epigenetic Memory Persistence: The biological phenomenon where specific chromatin regions remain physically accessible despite the cessation of active inflammation and the return of normal gene expression.
• Stem Cell Inheritance: The mechanism by which strong epigenetic alterations are passed from intestinal stem cells to their descendant "daughter" cells across multiple generations of cell division, creating entire lineages primed for malignancy.
• The "One-Two Punch" Model: The synergistic requirement of both an initial environmental/epigenetic alteration and a later genetic mutation to rapidly drive cancer progression.

Why cells respond “incorrectly” in old age

G. V. Shivashankar (left) and Yawen Liao from the PSI Center for Life Sciences have investigated how chromatin in human cell nuclei changes with age.
Photo Credit: © Paul Scherrer Institute PSI/Markus Fischer

Scientific Frontline: Extended "At a Glance" Summary: Chromatin Alteration in Cellular Aging

The Core Concept: As human cells age, the packaged form of DNA within the cell nucleus, known as chromatin, undergoes structural degradation and physically opens up. This alteration causes older cells to respond weakly or incorrectly to external mechanical and biochemical stimuli, leading to impaired cellular function.

Key Distinction/Mechanism: Unlike young cells, where tightly packed chromatin effectively restricts access to irrelevant genes, the relaxed chromatin structure in older cells fails to act as an accurate filter. When subjected to mechanical tension or growth factors (such as TGF-β), this disorganized state triggers incorrect gene expression, resulting in the production of unwanted proteins instead of those necessary for appropriate cellular responses.

Major Frameworks/Components:

• Chromatin Architecture: The three-dimensional structural packaging of DNA that regulates genome accessibility for transcription.
• Cellular Mechanotransduction: The mechanism through which cells translate mechanical forces (such as tension within a 3D collagen matrix) into biochemical signals and genetic responses.
• Aberrant Gene Expression: The age-induced misregulation where previously inaccessible, irrelevant genes are inappropriately activated due to chromatin degradation.

The influence of lymph node architecture on lymphoma

Professor Dr Sascha Dietrich (Director of the Department of Hematology, Oncology and Clinical Immunology) emphasises that the targeted modulation of stromal cells offers great therapeutic potential for the treatment of malignant lymphomas.
Photo Credit: © UKD

Scientific Frontline: Extended "At a Glance" Summary: The Influence of Lymph Node Architecture on Lymphoma

The Core Concept: Stromal cells function as the "architects" of lymph nodes by directing immune cells via chemical signals, but during the development of B cell lymphomas, inflammatory feedback loops reprogram these cells, actively destroying the lymph node's structural organization.

Key Distinction/Mechanism: Unlike the passive displacement of tissue by tumor growth, the structural breakdown in aggressive lymphomas (such as diffuse large B cell lymphoma) is an active process. T cell-produced interferons force stromal cells to replace structure-defining chemokines with inflammatory ones, attracting more inflammatory cells and obliterating the spatial boundaries that remain largely intact in slower-growing lymphomas (such as follicular lymphoma).

Major Frameworks/Components:

• Stromal Cell Regulation: Non-haematopoietic structural cells that normally release chemokines to organize B cells and T cells into specific zones.
• Inflammatory Feedback Loop: The active mechanism where T cells produce interferons in the tumor microenvironment, fundamentally altering stromal chemokine production.
• Advanced Tissue Mapping: The utilization of single-cell analyses and spatial tissue mapping to trace the progressive loss of regulatory signals.

Prehistoric fish: coelacanths heard underwater using their lungs

3D rendering of the skeleton of Graulia branchiodonta. The auditory organ includes the bony wings (red) on the ossified lung (white) which transmitted sound vibrations to the inner ear (not shown) located in the prootic bone in the skull (pink).
Image Credit: © L. Manuelli–MHNG

Scientific Frontline: Extended "At a Glance" Summary: Prehistoric Coelacanth Auditory Systems

The Core Concept: Some 240-million-year-old ancient coelacanths utilized an ossified lung as a specialized sensory organ to detect and process underwater sound.

Key Distinction/Mechanism: Unlike modern deep-sea coelacanths that rely exclusively on gills for respiration and lack this auditory adaptation, these Triassic ancestors possessed an air-filled, ossified lung equipped with wing-like bony extremities. Underwater sound waves captured by the lung were transmitted through a specialized canal directly to the inner ear. This mechanism is functionally analogous to the Weberian apparatus found in modern freshwater fish, such as carp and catfish, where a swim bladder amplifies acoustic vibrations.

Major Frameworks/Components: 

• Synchrotron Imaging: High-resolution, micrometric X-ray imaging conducted at the European Synchrotron Radiation Facility (ESRF) used to non-destructively map the internal anatomy of the fossils.
• Ossified Lung Structure: An ancient anatomical feature covered in overlapping bony plates, previously thought to be strictly an adaptation for air breathing.
• Acoustic Transmission Canal: A newly identified neural and structural pathway connecting the hearing and balance organs in the skull to the ossified lung.
• Evolutionary Regression: The eventual loss of this auditory system as modern coelacanth ancestors adapted to deep marine environments, rendering the specialized lung unnecessary.