Biology (9700) Exam Tips

The 5-Minute Habit That Saves a Whole Grade

Entering the Cambridge International AS Level Biology exam room can feel overwhelming, but top-performing students rely on a highly deliberate 5-minute reading routine. Before writing a single word on Paper 2 or Paper 3, scan the entire paper. This habit prevents the classic mistake of jumping to conclusions. For instance, when asked to complete a diagram of anaphase, many candidates fail to read the fine print and draw too many chromosomes (such as 11 pairs instead of a single pair for chromosome 11), costing easy marks. By scanning ahead, you allow your brain to unconsciously process the questions, plan your space, and budget your time effectively.

Time management across the papers is strict. For Paper 1 (Multiple Choice), you have 75 minutes for 40 questions—aim for roughly 1.5 minutes per question, leaving 15 minutes at the end to double-check tricky questions. For Paper 2 (Structured Questions), you have 75 minutes for 60 marks, meaning a strict 1.2 minutes per mark. If a question is worth 3 marks, do not spend more than 3 to 4 minutes on it. In Paper 3 (Advanced Practical Skills), you have 120 minutes for 2 questions (20 marks each). You must dedicate the first 60 minutes to Question 1 (usually the wet lab biochemical or transport investigation) and the remaining 60 minutes to Question 2 (microscopy and biological drawing). If your water bath is heating up, use that idle time to complete table headers and calculations rather than waiting passively.

Where the Marks Really Hide: The Precision of Terminology

In AS Level Biology, generalities are the enemy of marks. Cambridge examiners use highly specific mark schemes where vague language is strictly penalized. One of the most recurring pitfalls is the casual use of the term "cell membrane." You must specify "cell surface membrane" or "plasma membrane" when referring to the outermost boundary of an animal cell or the site of active transport. Referring to a capillary endothelium as having a "cell wall" or using "cell membrane" instead of "cell surface membrane" will immediately result in a loss of marks.

This demand for precision extends to other biological systems as well:

• Biochemical Names: Watch your spelling closely. Mistaking thymine for thiamine (a vitamin) or cytosine for cysteine (an amino acid) will cost you the mark. When describing DNA transcription, ensure you refer to the molecule from which introns are removed as the "primary transcript" rather than "mRNA."
• The Chloride Shift: When discussing the transport of respiratory gases in blood, always include the word "ion". You must write "chloride ions" and "hydrogencarbonate ions." Omitting the word "ion" is mathematically and scientifically incorrect.
• Myogenic Heart Control: Never use general words like "contraction and relaxation" if the question instructs or implies the use of cardiac cycle terminology; use "systole" and "diastole". When detailing the pathway of electrical impulses, explicitly state that the atrioventricular node (AVN) introduces a 0.1-second delay to allow the atria to fully empty before the ventricles contract, and note the role of the non-conducting fibrous ring (annulus fibrosus) in preventing impulses from spreading directly.
• Gaseous Exchange Structures: Do not confuse smooth muscle with elastic tissue. Smooth muscle in the bronchus or arteriole wall contracts and relaxes to adjust lumen diameter, whereas elastic fibres/elastic tissue stretch and recoil to accommodate changes in volume or expel air.

Slaying the Math: Magnification and Dilutions Without Tears

Quantitative analysis constitutes a large portion of your final grade. The formula for magnification is a fundamental tool: \( M = \frac{I}{A} \) (Magnification = Image size / Actual size). Marks are consistently lost because students struggle with unit conversions or fail to show their working. Always use this foolproof process:

1. Measure the image size (I) with a ruler in millimeters (mm).
2. Convert this measurement into micrometers (\( \mu \text{m} \)) by multiplying by 1000 (e.g., \( 24 \text{ mm} \times 1000 = 24,000 \text{ } \mu \text{m} \)).
3. Divide by the actual size (A), which is usually given in micrometers (e.g., \( 2 \text{ } \mu \text{m} \)). \( M = \frac{24,000}{2} = \times 12,000 \).
4. State your final answer to the requested number of significant figures (usually 3).

In Paper 3, you will frequently be asked to perform a serial dilution. If you are preparing a simple halving serial dilution (e.g., from 1.0% to 0.5%, 0.25%, 0.125%, and 0.0625%), you must show clear arrows representing the volume of solution transferred (e.g., 10 \( \text{cm}^3 \)) and the volume of distilled water added (10 \( \text{cm}^3 \)) to each beaker. Always ensure your table headers contain both the variable name and its unit separated by a forward slash (e.g., Percentage concentration of glucose / % or Time / s). Never write units inside the data cells themselves; they belong strictly in the header row.

The Art of the Pencil: How to Draw for Maximum Marks

Your biological drawings in Paper 3 are evaluated on strict technical rules. Examiners are not looking for artistic masterpieces; they are looking for precise, anatomical records.

• No Shading or Sketching: Use a sharp HB pencil. Draw clean, single, continuous lines. Fuzzy, overlapping, or shaded lines are heavily penalized.
• Low-Power Tissue Plans: When asked to draw a low-power plan diagram (e.g., of a root or stem section), do not draw any individual cells. Only draw the boundaries of the tissue layers. If you draw even one cell, you risk losing all format marks.
• High-Power Cellular Drawings: When drawing adjacent plant cells, you must represent the thick cell walls by drawing double lines. Ensure adjacent cell walls touch where appropriate and that your lines close completely.
• Label Lines: Use a ruler to draw straight, solid label lines that end precisely on the target structure. Do not use arrowheads, and never cross your label lines.

What Top Scorers Do Differently: Thinking in Systems

The highest-scoring candidates do not just memorize facts; they understand how biological systems interact. For example, when discussing enzymes, they can clearly contrast Emil Fischer's legacy lock-and-key hypothesis with the modern induced-fit mechanism. They explain that under induced-fit, the active site is only partially complementary to the substrate initially, and that binding causes a conformational change in the active site shape, molding it around the substrate to form a tight, stable enzyme-substrate complex (ESC) and lowering the activation energy.

Top scorers also pay close attention to biochemical terminology. They know that penicillin works by binding to and inhibiting the transpeptidase enzyme, preventing the formation of new peptide cross-links in peptidoglycan cell walls during bacterial growth, rather than "breaking" or "digesting" existing walls. Developing this level of detail in your study routine will elevate your performance from a basic pass to an outstanding top grade.